Hostname: page-component-76fb5796d-vvkck Total loading time: 0 Render date: 2024-04-26T16:46:47.651Z Has data issue: false hasContentIssue false
  • English
  • Français

Potential long consequences from internal and external ecology: loss of gut microbiota antifragility in children from an industrialized population compared with an indigenous rural lifestyle

Published online by Cambridge University Press:  24 May 2023

Isaac G-Santoyo ,
Elvia Ramírez-Carrillo Open the ORCID record for Elvia Ramírez-Carrillo [Opens in a new window] ,
Jonathan Dominguez Sanchez  and
Oliver López-Corona
Isaac G-Santoyo*
Affiliation:
Neuroecology Lab, Department of Psychology, UNAM, México, 04510 Unidad de Investigación en Psicobiología y Neurociencias, Department of Psychology, UNAM, México, 04510
Elvia Ramírez-Carrillo*
Affiliation:
Investigadores por México (IxM)-CONACyT, Facultad de Psicología, UNAM, México, 04510
Jonathan Dominguez Sanchez
Affiliation:
Neuroecology Lab, Department of Psychology, UNAM, México, 04510
Oliver López-Corona*
Affiliation:
Investigadores por México (IxM)-CONACyT, Instituto de Investigaciones en Matemáticas Aplicadas y en Sistemas (IIMAS), UNAM, México, 04510
*
Corresponding author: Isaac G-Santoyo, Neuroecology Lab, Department of Psychology, UNAM, México, 04510. Email: isantoyo@psicologia.unam.mx; Elvia Ramírez-Carrillo, Investigadores por México (IxM)-CONACyT, Facultad de Psicología, UNAM, México, 04510. Email: elviarc@otrasenda.org; Oliver López-Corona, Investigadores por México (IxM)-CONACyT, Instituto de Investigaciones en Matemáticas Aplicadas y en Sistemas (IIMAS), UNAM, México 04510. Email: lopezoliverx@ciencias.unam.mx
Corresponding author: Isaac G-Santoyo, Neuroecology Lab, Department of Psychology, UNAM, México, 04510. Email: isantoyo@psicologia.unam.mx; Elvia Ramírez-Carrillo, Investigadores por México (IxM)-CONACyT, Facultad de Psicología, UNAM, México, 04510. Email: elviarc@otrasenda.org; Oliver López-Corona, Investigadores por México (IxM)-CONACyT, Instituto de Investigaciones en Matemáticas Aplicadas y en Sistemas (IIMAS), UNAM, México 04510. Email: lopezoliverx@ciencias.unam.mx
Corresponding author: Isaac G-Santoyo, Neuroecology Lab, Department of Psychology, UNAM, México, 04510. Email: isantoyo@psicologia.unam.mx; Elvia Ramírez-Carrillo, Investigadores por México (IxM)-CONACyT, Facultad de Psicología, UNAM, México, 04510. Email: elviarc@otrasenda.org; Oliver López-Corona, Investigadores por México (IxM)-CONACyT, Instituto de Investigaciones en Matemáticas Aplicadas y en Sistemas (IIMAS), UNAM, México 04510. Email: lopezoliverx@ciencias.unam.mx
Rights & Permissions [Opens in a new window]

Abstract

Human health is strongly mediated by the gut microbiota ecosystem, which, in turn, depends not only on its state but also on its dynamics and how it responds to perturbations. Healthy microbiota ecosystems tend to be in criticality and antifragile dynamics corresponding to a maximum complexity configuration, which may be assessed with information and network theory analysis. Under this complex system perspective, we used a new analysis of published data to show that a children’s population with an industrialized urban lifestyle from Mexico City exhibits informational and network characteristics similar to parasitized children from a rural indigenous population in the remote mountainous region of Guerrero, México. We propose then, that in this critical age for gut microbiota maturation, the industrialized urban lifestyle could be thought of as an external perturbation to the gut microbiota ecosystem, and we show that it produces a similar loss in criticality/antifragility as the one observed by internal perturbation due to parasitosis by the helminth A. lumbricoides. Finally, several general complexity-based guidelines to prevent or restore gut ecosystem antifragility are discussed.

Keywords

Gut microbiotaantifragilitylifestylescriticalityecology
Type
Original Article
Information
Journal of Developmental Origins of Health and Disease , Volume 14 , Issue 4 , August 2023 , pp. 469 - 480
Check for updates
Creative Commons
Creative Common License - CCCreative Common License - BY
This is an Open Access article, distributed under the terms of the Creative Commons Attribution licence (http://creativecommons.org/licenses/by/4.0/), which permits unrestricted re-use, distribution and reproduction, provided the original article is properly cited.
Copyright
© The Author(s), 2023. Published by Cambridge University Press in association with International Society for Developmental Origins of Health and Disease

Introduction

The introduction discusses the complexity of the gut microbiota, which is composed of thousands of bacterial species that self-organize to exhibit non-trivial global structures and behaviors. Two main characteristics of complex systems – emergence and self-organization – are described, and it is explained how complexity can be considered a balance between these two factors. The concept of criticality is introduced, which is a scale-invariant dynamical regime that maintains a balance between flexibility and robustness in a system. Criticality is present in all living systems and is associated with maximum inference and computational capabilities. We propose that complexity is a universal payoff function of living systems and may be used in the measurement of both criticality and antifragility. Please see the glossary in the supplementary materials.

The gut microbiota is an ecosystem mainly composed of thousands of bacterial species that, through local interactions with each other, self-organize to exhibit non-trivial global structures and behaviors at larger scales, giving place to properties that may not be understood or predicted from the full knowledge of the species biology alone. These properties are acknowledged in the standard definition of a complex system, and it is well recognized that new mathematical frameworks and scientific methodologies are required for their understanding. Reference Domenico, Brockmann and Camargo1

Two of the main characteristics of complex systems are Emergence and Self-organization. Emergence is the information that results in a system after being subjected to any process that modifies it. This information is only observable when all elements of the system are included, and it can be mapped and measured by Shannon information (S). On the other hand, Self-organization can be considered as the magnitude of change in the system order over time, Reference Gershenson and Heylighen2 and it is usually seen as the opposite of emergence since whenever the system increases organization, information diminishes. In that sense, Complexity (C) can be considered as the product of emergence and self-organization, somehow encoding a balance between processes that generate information and randomness with processes that generate order-reducing information. Reference Gershenson and Fernández3

In terms of dynamics, this translates into a balance between flexibility and robustness Reference Huitzil, Sandoval-Motta, Frank and Aldana4 that usually evolve into a scale-invariant dynamical regime called criticality. This property is present in all living systems, Reference Hidalgo, Grilli and Suweis5 where the maximum inference and computational capabilities are achieved. Reference López-Corona and Padilla6

Criticality is, in consequence, a state that maintains the system in an equable trade-off between flexibility and robustness in a specific scale of observation. Hence, it is expected that the criticality regime would be observed as part of what we consider health in a system. For instance, there is cumulative empirical evidence that in young and healthy individuals, both the heart and brain are in criticality Reference Goldberger7-Reference Rivera, González-Montoro and Alberola-López10 ; on the opposite side of the coin, under conditions of elderly or chronic diseases (such as obesity or diabetes), there is a loss of criticality mainly by loss of flexibility/emergence. Reference Goldberger, Amaral and Hausdorff11 There is also solid evidence that gene regulatory networks of natural organisms are in or close to criticality. Reference Schmulevich, Dougherty and Kim12-Reference Daniels, Kim and Moore15

Taking into consideration the ecosystems formed by the microbiota, and from a more general network theory perspective, Huitzil and co-workers Reference Huitzil, Sandoval-Motta, Frank and Aldana4 have proposed that microbiota ecological networks are critical, Reference Derrida and Pomeau16 conferring the system evolvability Reference Aldana17,Reference Aldana, Balleza, Kauffman and Resendiz18 that enhances faster information storage, processing, and transfer. Reference Langton19,Reference Nykter, Price and Larjo20 This informational capability means that healthy microbiota ecosystems are able to respond to external perturbations. Reference Kinouchi and Copelli21 For instance, recent work has shown that greater network complexity is related to higher resilience to perturbation by microbiota communities Reference Karimi, Maron and Chemidlin-Prevost Boure22 and that more complex microbial networks are characteristic of the least disturbed (external) ecosystems, as shown in soil microbial networks that reduce their complexity when agriculture intensifies. Reference Banerjee, Walder and Büchi23

On the other hand, microbiota ecosystems (and ecosystems in general) could also and must do much more than merely respond to environmental perturbations; they most certainly have built-in characteristics that enable them to even take advantage of them. Antifragility is maybe the core one of these characteristics Reference Danchin, Binder and Noria24,25 ; which is the exact opposite of fragility (being broken by randomness, perturbations, or time) and is defined by Taleb as the nonlinear locally convex response of a specific payoff function in front to a well-defined perturbation, in terms of type, intensity or frequency (i.e., A formal definition of antifragility as convexity in the payoffs space is found in Taleb & Douady Reference Taleb and Douady26 and Taleb. Reference Taleb27

As we have eco-evolutionary reasons and empirical evidence that strongly support the idea that all living systems tend to criticality in which complexity (balance of Emergence and Self-organization) and Fisher information (system stability) are maximum, meaning that they have the best computational and inferential capabilities, then any deviation from criticality (depart from maximum complexity) must result in a diminishing of the system capabilities to respond to perturbations. So, one may consider that complexity is a universal payoff function for living systems and may be used in the measurement of criticality and antifragility. Reference López-Corona and Padilla6,Reference Ramírez-Carrillo, López-Corona and Toledo-Roy28,Reference Equihua, Aldama and Gershenson29

A gut ecosystem perturbation might come from internal and external factors. For instance, it is known that gut parasites could be a source of internal perturbation, since they produce changes in physiological processes, including hormonal, Reference Romano, Jiménez, Miranda-Brito and Valdez30 neurological, Reference Johnson and Nath31 and immunological Reference Shepherd, Navarro and Wangchuk32 processes, that can even affect the host’s behavior; for example, the parasitic wasp cotesia congregata induces the host manduca sexta to increase the octopamine concentration in its hemolymph, then the frontal ganglion’s motor pattern is disrupted by the elevated octopamine concentration, which prevents food intake. Reference Adamo33,Reference González-Tokman, Córdoba-Aguilar, González-Santoyo and Lanz-Mendoza34 Evidence points out that, to some extent, not only micro but also macro-organisms in the gut are capable of modifying several physiological axes of the host. In recent work Reference Ramírez-Carrillo, López-Corona and Toledo-Roy28 authors found compelling evidence that suggests the presence of the gut parasite Ascaris lumbricoides induced perturbations in human gut microbiota network properties, translating to a loss of emergence, a departure from criticality, and ultimately loss of health.

On the other hand, external perturbations may come from different sociocultural practices present in a particular lifestyle and in the ecological conditions in which the individual is living. Both external factors are essential during childhood since, during this period, the human gut microbiota is more sensitive to perturbations, which affects its stability and maturity. Reference Olm, Dahan and Carter35,Reference Sonnenburg and Sonnenburg36

Different environments and behaviors have influenced the evolution of the human microbiota throughout human evolutionary history, and it has become an essential line of research in which multiple studies have compared the gut microbiota of industrialized versus non-industrialized (i.e., traditional and rural) human populations. Reference Sonnenburg and Sonnenburg36,Reference Rosas-Plaza, Hernandez-Teran and Navarro-Diaz37 As a result, it has been found that gut microbiota might be very vulnerable to industrialization.

For example, cultural strategies to kill or limit exposure to pathogenic microbes, such as broad-spectrum antibiotics and sanitation, or the consumption of ultra-processed foods containing preservatives and additives, could act as selective forces for gut microbiota favoring certain groups but affecting others. Consequently, the gut microbiota of individuals living in industrialized societies is less rich and diverse than that of individuals living in non-industrialized societies. Also, this last lifestyle shares taxa that have been lost or reduced, such as members of the Spirochaetes or Prevotellaceae family. Reference Sonnenburg and Sonnenburg36,Reference Sanchez-Quinto, Cerqueda-Garcia and Falcon38

The changes in the micro-ecosystem configuration as a product of industrialization might affect the host´s health due to the subsequent loss of the ecosystem services offered. The gut microbiota intervenes in the maturation and regulation of the immune system, the synthesis of vitamins and hormones, food digestion, protection against pathogens, etc. Hence, the relationship between gut microbiota and several chronic diseases mainly present in industrialized societies has become more evident. The evidence of this relation has been mainly constructed by either evaluating specific species isolated from the rest of the gut microbial ecosystem, or by measuring its composition, structure, and diversity under classical ecological lenses. Reference Selber-Hnativ, Korem and Segal39-Reference Ramírez-Carrillo, Gaona and Nieto41 However, these approaches could underestimate ecosystem emergence and self-organization, both important not only to quantify the current health state of the microbiota (and its host) but also, its ability to respond to subsequent perturbations. In that sense, a scenario that includes internal and external sources of perturbations, such as lifestyles or parasites, may set an excellent ecologically valid experiment to determine differences or similarities regarding the criticality/antifragility of gut microbiotas that have been shaped under these conditions.

Furthermore, microbes in the gut ecosystem interact with each other in non-trivial ways including the use of intermediary molecules, metabolites, and/or toxins, Reference Kim and Price42-Reference Fernandez, Riveros, Campos, Mathee and Narasimhan47 yet the exact nature of each interaction and more importantly its measurement is usually inaccessible using standard methods. So, as pointed out by Cickovski and co-workers, Reference Cickovski, Peake, Aguiar-Pulido and Narasimhan48 an alternative method to assess this interaction is to measure bacterial co-occurrence networks, which has been widely applied in exploring the potential interactions among microbes. Reference Banerjee, Walder and Büchi23,Reference Ackerman44,Reference Fernandez, Riveros, Campos, Mathee and Narasimhan47,Reference Atkinson and Williams49,Reference Jiao, Wang, Wei, Chen and Lu50 In very general terms, a co-occurrence network is an undirected, weighted network with nodes that represent bacterial taxa present in the community and edges that correspond to how strongly the two taxa tend to co-occur (i.e., co-infect) in the sampled communities.

Therefore, using a novel perspective of complex systems, we evaluate the criticality/antifragility of gut microbiotas from children subjected to an external perturbation promoted by an industrialized lifestyle and an internal perturbation promoted by the presence of the gut parasite Ascaris Lumbricoides. In this work we are using the labels “external “and “internal” in relation to (1) the ecological perturbations that come from the ecosystem where the individuals live in form of their diet regimes (as part of a specific lifestyle); and, (2) the ecological perturbations that come from the conditions of the gut microbiome ecosystem inside the individuals. This labeling, used basically to remind the reader that we are working with two different types of ecosystems, should not be interpreted as if we are equating industrialized lifestyle and the presence of parasites.

Methods

Study subjects

We study two populations of children from 5 to 10 years old under two sources of perturbations. The first one, living in a non-industrialized rural indigenous population located in southwest Mexico, was under the influence of an internal source caused by the presence of the gut parasite A. lumbricoides. The second one was affected by an external perturbation induced by the contrasting lifestyle lead in an urban population in Mexico City.

The geographical region called “la Montaña Alta” in Guerrero, México, has an essential history of economic marginalization. In particular, the Me'phaa indigenous communities have access to a homogeneous and limited variety of diets and depend on subsistence farming and seasonal foods. Reference Barragán51 Data from the federal office that evaluates poverty and socioeconomic development (i.e., CONEVAL) point out that in 2018, 27.8% of the population in Guerrero was below the threshold of food insecurity; 93% of this population was located in two regions, “montaña alta” and “montaña baja.”

We obtained the rural samples from two Mephaa communities; “Plan de Gatica” (17°7′ 49.5552″ N, 99.7′ W, EASL 510 m) and “El Naranjo” (17°9'54.0036" N 98°57', 50.9832" W, EASL 860 m); both communities are part of the geographical region of “the Montaña Alta” in Guerrero (see Fig. 1) and 56 km away from each other.

Figure 1. Locations of Plan de Gatica and El Naranjo, indigenous localities located in the municipality of Ayutla de los Libres and Acatepec (respectively) in the Montaña Alta region of the state of Guerrero, México. Families of these locations were the study subject of this research.

The 2020 Population and Housing Census conducted by the National Institute of Statistics and Geography shows that the inhabitants of both communities are exclusively indigenous, and are within the regions with the greatest poverty and social vulnerability in Guerrero and the entire country. Thus, the consensus in the municipality that includes the “Plan de Gatica” community has 28.4% of individuals living in extreme poverty (20,998 people). Similarly, 67.75% of the people from “Acatepec,” the other municipality that includes the “El Naranjo” community, live in the same poverty conditions.

These indigenous people generally dwell in settlements of fifty to eighty households, each with five to 10 individuals. Most residents only speak “Me’phaa,” their native language, and they mainly depend on subsistence farming of legumes such as beans and lentils, with corn being the primary grain grown. In addition to gathering wild edible plants, some fruits and vegetables are grown in garden plots. Reference Borda-Niño, Hernández-Muciño and Ceccon52 Hunting and rearing some poultry provide animal protein, but the consumption of this food is primarily on special occasions, such as festivities; hence it is not a regular food in the diet of the “Me’Phaa” people. Reference Borda-Niño, Hernández-Muciño and Ceccon52

In contrast, the samples from the city group comprise children from the southern area of Mexico City (18.102" W 19°12'36.36" W). This urban population is essentially the opposite of the indigenous population mentioned above. The children of urban dwellers lead a Western lifestyle that is comparable to that of upper-middle class families, who routinely consume diets based on ultra-processed foods and animal-products consumption; refined products, such as oils, sugar, salts, and grains; as well as low consumption of whole grains, fiber, and vegetables. Additionally, they have easy access to allopathic medications, such as antibiotics and other medications.

It is important to highlight that the urban population does not present parasites and that previous work Reference Ramírez-Carrillo, Gaona and Nieto41 suggests that the presence of Ascaris lumbricoides in the rural population can cause a perturbation in the gut microbiota network, leading to a loss of emergence and departure from criticality, ultimately resulting in a loss of health. This highlights the importance of studying the interactions between gut microbiota and parasites and their potential impact on human health. The study also demonstrates the usefulness of network analysis techniques in understanding these complex interactions. The practical implications of this research could include the development of new strategies for managing and treating parasitic infections and their associated health effects.

The non-industrialized Rural (R) population in this study consists of 29 children; 18 Non-Parasitized (NP) and 11 Parasitized (P), all of them belong to the Me´phaa population. The Urban (U) population considers 13 children all NP from México City, who practice a clearly industrialized style of life. Parasites were determined following the protocol implemented in Ramírez-Carrillo et al. Reference Ramírez-Carrillo, Gaona and Nieto41

The Rural population has a particular set of historical conditions that make it the more contrasting group in terms of lifestyle in regard to typical urbanized areas of Mexico City. Reference Black53-Reference Miramontes, DeSouza, Hernández and Ceccon55

Due to the socioeconomic context of this population, associated with historic poverty and marginalization, they have the lowest income and the lowest access to health services in the country. In terms of biological path dependence, this population has almost no access to allopathic medications that we know and that may have induced important changes in the microbiota ecosystem. Reference Camacho54,Reference Doorduyn, Van Den Brandhof, Van Duynhoven, Wannet and Van Pelt56-Reference Hernández-Muciño, Borda-Niño and Santiago59 Although allopathic medication is practically absent in these communities Reference Hernández-Muciño, Borda-Niño and Santiago59,60 we selected only participants that had not taken any medications such as antibiotics or anthelmintic treatment during the two years prior to the study.

Finally, Lewis et al. Reference Lewis, Obregón-Tito, Tito, Foster and Spicer61 argues that indigenous populations in research on the human microbiome are essential for several reasons. First, indigenous populations often have unique microbiomes due to differences in diet, lifestyle, and environmental exposures, which can provide valuable insights into the factors that shape the human microbiome. Second, indigenous populations have a long history of traditional medicine practices that often involve the use of microbial communities, which can inform new approaches to microbiome-based therapies. Third, the participation of indigenous communities in microbiome research can help to address health disparities and promote health equity by identifying microbiome-based interventions that are effective in diverse populations. Overall, the inclusion of indigenous populations in microbiome research is essential in increasing our understanding of the human microbiome and developing new interventions for improving human health.

Taxonomic bacterial inference

For this work, as explained in more detail by Ramírez-Carrillo and co-workers (2020), gut microbiota taxonomic inference was obtained from fecal samples through High Throughput Sequencing in the Illumina platform. Briefly, each participant provided a fecal sample in a sterilized plastic bottle, which was frozen with liquid nitrogen in subsequent storage at −20°C, until DNA extraction. After extraction, the V4 hypervariable region of the 16S rRNA gene (ribosomal ribonucleic acid) was amplified with the universal bacterial/archaeal primers 515F/806R. Characterization of fecal purified 16S rRNA fragments (20 ng per sample) was sequenced on an IlluminaMiSeq platform and paired-end reads of around 250 bp were generated. These readings were processed in QIIME2, noise was removed with the DADA2 complement to obtain the Amplicon Sequence Variants (ASVs). Through filters and comparisons with databases, tables of abundance and phylogeny of the representative ASVs were made.

ASVs represent the biological sequences of the 16S rRNA gene and distinguish sequence variants that differ by as little as one nucleotide between each sample. Reference Callahan, McMurdie and Holmes62 Abundance and phylogeny data were analyzed under R environment using phyloseq Reference McMurdie and Holmes63 and ggplot2 packages. 21,000 reads per sample were used as the minimum sequencing effort for Plastidic ASVs filtering. Sequence data is available in the NCBI database with Bioproject number PRJNA593240. 64 All the testing and recruitment procedures of the study were approved (September 25, 2017) by the Research Ethics Committee of the Faculty of Psychology of the National Autonomous University of Mexico (FPSI/CE/01/2016) and were executed in accordance with the ethical principles and guidelines of the Official Mexican Law (NOM -012-SSA3-2012). The persons responsible for the care of participating infants read and signed a written informed consent.

Network modeling and complexity estimation

In this work, we construct a co-occurrence matrix from the ASVs dataset (i.e., bacteria species) using the Cooccur package Reference Oksanen65 (https://cran.r-project.org/web/packages/cooccur/cooccur.pdf) in R (74) for the three populations under study.

Although the network theory approach has shown to be most useful in a number of contexts Reference Todd66-Reference Neel and Orrison69 and the concept of network complexity is central, there is still a lack of a universally accepted measure of complexity. Reference Dehmer, Emmert-Streib, Graber, Salvador and Shi70-Reference Mowshowitz and Dehmer72 Among many possible measures of network complexity, the entropy-based ones including number of vertices, number of neighbors, and number of neighbors at a given distance have been recognized to be both simple to use and useful. Reference Cao, Dehmer and Shi73 For this, we used the CytoHubb app inside CytoScape, Reference Shannon, Markiel and Ozier74 an open-source Network Analysis software, to calculate the average number of neighbors, number of nodes, and Network heterogeneity which as we have commented are related to different aspects of complexity. Additionally, to determine complexity directly we calculate the Shannon information (S), which is a proxy of informational emergence, Reference Gershenson and Fernández3 for each individual of the population Rural-P (R-P), Rural-NP (R-NP), U.

As was pointed out before, this study considered an indigenous community that depends on traditional agriculture and foraging; and an urban community that relies on industrialized food production. The rationale for choosing two communities with contrasting subsistence models is that these dissimilarities were expected to lead to differences in the gut microbiome of the two groups, as diet is a significant determinant of gut microbiome composition. In order to compare the gut microbiome of the two groups, fecal samples were collected from each participant and analyzed using 16S rRNA gene sequencing to identify the bacterial species present in their gut microbiome. The researchers also collected information on the children’s diets and lifestyles through surveys and interviews.

Overall, the sample design was devised to test the hypothesis that different subsistence models lead to differences in gut microbiome composition, intending to improve our understanding of how diet and lifestyle factors influence the gut microbiome.

Results

In general terms, the current work describes a study case that analyzes the gut microbiota networks of three populations: U, R-NP, and R-P. The study uses The Graph Edit Distance (GED) analysis, to compare the complete network structures of the three populations. The higher the value of GED, the more dissimilar the networks are.

In particular, Fig. 2 shows the GED analysis score of the gut microbiota ecosystem network for the R-NP group (considered the control group for comparison) and the two under perturbation (R-P and U-NP). The results indicate that U and R-P characteristics affect gut microbiota networks in a similar manner, suggesting that U lifestyle could be thought of as a perturbation that may lead to similar patterns of microbiota dysbiosis.

Figure 2. We show the GED analysis score of gut microbiota ecosystem network for the Rural-NP group (considered as the control group for comparison) and the two under perturbation (Rural-P, Urban NP).

Fig. 3 shows three standard network metrics related to complexity and discusses them in terms of heterogeneity, highlighting the balance nature of complexity.

Figure 3. Network metrics usually associated with connectivity for the three populations.

Fig. 4 shows complementary network measurement metrics, while Fig. 5 shows the differences in Shannon Information (emergence) for the three populations. Both populations under perturbation, R-P and U, show a statistically lower value of Shannon information (emergence, diversity) than R-NP.

Figure 4. Complementary network measurements metrics.

Figure 5. Difference of Shannon Information (emergence) for the three populations (W = 162, p-value = 0.037). The box plot shows the median, quartiles, min-max, and point is the mean.

Overall, the study suggests that the U lifestyle could lead to similar patterns of microbiota dysbiosis as R-P and that the rural populations exhibit greater complexity in their gut microbiota networks than the urban population.

In more detail, Fig. 2 presents the results of The GED analysis, which compares complete network structures Reference Ibragimov, Malek, Guo and Baumbach75 for the three populations, U, R-NP and R-P. The higher the value of GED the more dissimilar the networks are. We see that the interval of GED between U and R-P is given by GED(U, R-P) <GED(U, R-NP) and GED(U, R-P) < GED(R-P, R-NP). So U and R-P characteristics affect gut microbiota networks in a similar manner. As it was previously reported, R-P corresponds to a perturbation that might produce a dysbiosis in gut microbiota, then U lifestyle could be thought of also as a perturbation that may lead also to similar patterns of microbiota dysbiosis.

In Fig. 3 we show three standard network metrics related to complexity. Both rural populations show greater values of the number of nodes and neighbors than urban (industrialized) populations. Between both rural populations, the R-NP exhibits greater values than R-P. We also found that urban microbiota networks are much more heterogeneous than rural ones, being the Parasitized the lowest. In general, systems that are either too heterogeneous or too homogeneous are less complex. Complexity is always manifested in the balance between self-organization (in this context homogeneity as a manifestation of the structuring that comes from order) and emergence (in this context heterogeneity as a manifestation of randomness).

Moreover, both populations under perturbation, R-P and U, show a statistically (Wilcoxon rank sum test one tail, W = 162, p-value = 0.037) lower value of Shannon information (emergence, diversity) than R-NP, as we can see in Fig. 5.

Discussion and conclusions

In a structural taxonomic approximation of these two children’s populations, Sanchez-Quinto et al Reference Sánchez-Quinto, Cerqueda-García and Falcón76 found that compared with children from Mexico City, the indigenous population showed higher alpha diversity in several indexes, such as Faith’s phylogenetic diversity, Shannon diversity, and observed ASVs. In addition, a subsequent beta diversity analysis indicated a clear separation between these two populations. In consequence, only a quarter (23.64%) of the total species (i.e., ASVs) were shared among the indigenous and urban populations (Fig. 6B; SUP); from these, 56 species showed statistically differentiated abundances, most of them overrepresented in the Me'phaa children.

Figure 6. Conceptual figure showing the effect of path dependence on the set of possible future configurations for gut microbiota ecosystem in terms of how it responds to perturbations to complexity as a general payoff function valid for systems under eco-evolutionary processes, and that define three types of configurations: fragility when it responds in a nonlinear concave way; robust if it is essentially insensible to perturbations or antifragile if it responds in a nonlinear convex way.

Related to a specific taxonomic structure, Firmicutes, Bacteroidetes, and Actinobacteria Phyla were more prevalent in children from México City than those from the Me'phaa (Supplementary Fig. 6H). Interestingly, several phyla were only found in the indigenous community in very low abundances, such as Deinococcus-Thermus (0.079%), Chloroflexi (0.01%), Elusimicrobia (0.01%), Acidobacteria (0.0071%), and Fibrobacteres (0.004%). (Supplementary Table S1) (Supplementary Fig. 6H).

In consequence, the GM composition and structure were remarkably different. These results are consistent with other studies that have pointed out the impact of lifestyle on GM. Reference Jha, Davenport and Gautam77-Reference Martínez, Stegen and Maldonado-Gomez82

Our results agree with Kaplan and co-workers. Reference Kaplan, Huttenhower, Pearce and Godfrey83 They found that Hispanic populations who immigrate early in life to the USA have low GM alpha diversity through the Shannon index, contrasting with those who relocate to the USA during adulthood, over 45 years old.

In that sense, our results contribute to the emergent concept of “social microbiome,” which suggests that interactions of social and ecological contexts that can take place at various levels of the biological organization may have an impact on the microbial exchange between organisms, and hence, in the states of GM ecosystems health.

We consider that by studying this interplay between lifestyles and GM ecosystems, we are starting to understand how the Holobiont co-evolves in a particular social context, in what we have proposed as a new eco-evolutionary ontological unit, named the ecobionts.

Returning to the discussion of standard analysis versus complex systems perspective, it is proposed that high GM taxonomic diversity is a proxy of GM health, since GM low-abundance great numbers of taxa are essential for the homeostasis and the constant maintenance of certain functions in human GM. Reference Arumugam, Raes and Pelletier84 Nevertheless, there are some valid critiques. Reference Roswell, Dushoff and Winfree85,Reference Konopiński86

For instance, a recent study on soil microbiome showed that its diversity and functionality can change under global environmental perturbations, but it does not always lead to microbial diversity loss. Furthermore, changes in land covered by agricultural practices increase alpha diversity. This seems to be occurring even during the conversions from highly diverse natural ecosystems to homogeneous agricultural monocultures, which is not a beneficial process for the original ecosystem.

In this sense, the ecosystem’s health is not only a function of composition, structure, and function in a particular moment, but it is also a function of how these attributes change over time and, more importantly, how they combine to allow the ecosystem to respond to perturbations, variability and ultimately to persist over time. In terms of how ecosystems respond to perturbations, there is information not contained in the composition and structure of its populations, but that emerges from several species interactions working together as a network. These properties of a biological system justify why a complex systems perspective using network theory is necessary and complements more standard analysis.

As with diversity in ecology, standard network theory metrics as heterogeneity do not map directly to criticality or antifragility, as has been discussed by López-Corona and co-workers Reference Ramírez-Carrillo, G-Santoyo and López-Corona87 who suggest that maximum antifragility arises at an “optimal” balance between homogeneity and heterogeneity that seems to be non-trivial, context-dependent, and in some cases, dynamic.

In that sense, this work implements the idea of how to use metrics from network theory to assess ecosystem antifragility which we have shown is a more general and rigorous conceptual framework to understand EH. Reference Equihua, Aldama and Gershenson29 Contrary to standard network metrics usually associated with criticality but in an indirect way, Minimum Spanning Tree has strong theoretical reasons Reference Van Dellen, Douw and Hillebrand88-Reference van Dellen, Sommer and Bohlken90 as well as empirical evidence associated Reference Stam, Tewarie and Van Dellen91 that prove why it is a valid metric to compare networks in terms of criticality/antifragility, and therefor is a promising metric for future works. For instance, we know that MST reflects global information transmission optimality (a requisite for criticality); it represents an informational backbone that has been diluted to the maximum possible level while maintaining connectivity. Specifically, its role as an informational backbone has been highlighted in recent applications. Reference Ramírez-Carrillo, G-Santoyo and López-Corona87,Reference Van Mieghem and van Langen92,Reference Saba, Premi and Cristillo93 Some applications of MST as an informational backbone include children with math difficulties, Reference Vourkas, Karakonstantaki and Simos94 dyslexic problems, Reference González, Van der Molen and Žarić95 amyotrophic lateral sclerosis disease, Reference Fraschini, Demuru and Hillebrand96 understanding sub-networks for the distinction of subject traits, Reference Crobe, Demuru, Didaci, Marcialis and Fraschini97 discrimination of motor imagery hand movement, Reference Demuru, Fara and Fraschini98 testing cognitive impairment in dementia, Reference Dauwan, Van Dellen and van Boxtel99 and to track some changes in the brain’s functional networks following surgery. Reference van Dellen, Sommer and Bohlken90

In the same line of thought, taking the new ideas about what an ecosystem is from a recent work about planetary antifragility, Reference López-Corona, Kolb, Ramírez-Carrillo and Lovett100 we consider that the GM is an open thermodynamic system constituted by a community of living organisms in conjunction with the nonliving components of their environment that is in health when through its interactions and evolutionary processes, constrained by the external conditions, self-organize into a criticality dynamic regime, with maximum computational and inferential capabilities that allow it to respond and thrive under uncertainty, stressors, perturbations and ultimately time, achieving maximum antifragility.

Even more, we could hypothesize that human systemic health arises from thermodynamic mechanisms that operate through human anatomy and physiology in its exchange of matter, energy, and information with its surroundings, until reaching an operational scale-invariant configuration in which there is an optimal balance, called Criticality; between order/robustness (self-organization) and random/flexibility (emergence) processes that confer the organism with the best capacities to respond and adapt to the environment, in what is called antifragility.

As suggested by Stuart A. Kauffman and others. Reference Hidalgo, Grilli and Suweis5,Reference Packard101-Reference Benedettini, Villani and Roli106 Life on a macroscopic scale displays a large amount of variability but it is much more uniform at the scale of cells, where all living systems share many common structural and functional features. How this macroscopic biodiversity emerges from the microscopic subsystems is explained by the principles of evolution, but even then, one may ask what natural selection chooses. A very promising basic principle to respond to that fundamental question is that evolution should have driven living beings toward critical states since they are favored by maximum computational and inferential capabilities called criticality; and which translate into system capacity to take advantage of environmental variability, randomness, and time, captured in the concept of Antifragility. Reference López-Corona and Padilla6,25

Traditionally, until recently, the vast majority of studies in gut microbiota focus on the relationship between some bacterial group and a specific pathology, comparing the abundances of species between samples or populations with some disease, versus a control sample; or through the relationship between the presence of certain bacteria and genetic properties of the host. These studies have generated a great deal of useful information by finding possible key relations with certain diseases, but these isolated analyses do not capture the complexity of the bacteria–bacteria interaction and bidirectionality between bacteria-hosts. This multi-scale dynamic set of interactions gives place to a very complex cascade of bacterial adaptations until a homeostatic balance is reached between the host and its microbiota. The new technical capabilities and analytical tools have made clear that the use of network theory promises to be a key piece in the future investigation of the complex relationship between the host and its gut microbiota. Reference Huitzil, Sandoval-Motta, Frank and Aldana4,Reference Coyte, Schluter and Foster107,Reference Layeghifard, Hwang and Guttman108

In this context, we have shown that the overall structure of the R-P (internal perturbation) microbiota network is 40% closer to U (external perturbation) than to R-NP (non-perturbed) population. We also found that the number of neighbors and nodes is the highest in the R-NP, followed by the R-P, and the lowest in the U population. These two-network metrics are directly related to the biodiversity in the microbiota ecosystem, and if taken together with the result that the U network is very heterogeneous, the R-P has a very low value of network heterogeneity and the R-NP has a middle value, we infer that the R-NP microbiota network is more complex than that in the perturbed populations. We know that complexity is lost whenever the system network heterogeneity is very high or low. In terms of Shannon information – a standard proxy of total richness and diversity, but also a system emergence Reference Gershenson and Fernández3 – we found that R-NP has a higher value that is statistically different from both R-P and U. As we know that R-P is a condition that might lead to dysbiosis due to the presence of parasites, Reference Kim and Price42 then the lower value of Shannon Information represents a lower complexity level and hence a loss in criticality/antifragility compared to R-NP. Thus the lower value of Shannon information for U is also a loss of complexity and criticality/antifragility.

Our work offers evidence that external perturbations in the form of U lifestyle may be considered equivalent to internal perturbations such as the presence of parasites; and that both lead to a loss of antifragility in the gut microbiota ecosystems. This result is consistent with recent studies that show that Industrialized populations exhibit a consistent loss of gut microbial diversity and also that they are clearly related to several non-communicable chronic diseases. Reference Smits, Leach and Sonnenburg109-Reference Tett, Huang and Asnicar114

Our results also adhere to the idea that microbiota in general plays a key role in host evolution and ecology and particularly that the gut microbiota acts as a fast response network coupled with a slow response one, the genome, that confers evolutionary criticality. In this sense, there is accumulated evidence that industrialized lifestyles have rapidly changed the human gut microbiota ecosystem which translates into high rates of these Noncommunicable diseases. Reference Huitzil, Sandoval-Motta, Frank and Aldana4,Reference Smits, Leach and Sonnenburg109,Reference Sandoval-Motta, Aldana and Frank115 We now know that some kind of “extinction event” in human gut bacteria might have already happened involving the loss of some species, such as Ruminococcus callidus, Butyrivibrio crossotus, and T. succinifaciens; and the increase in the number of Bacteroides and Prevotella SGBs Reference Wibowo, Yang and Borry116 ; the direction and changes of the different functional groups in the gut microbiota ecosystem may still remain far from being fully understood.

Growing evidence suggests that recent lifestyle changes, most notably the high-fat, high-sugar “Western” diet, have affected the genetic makeup and metabolic processes of the human gut microbiome. Reference Turnbaugh, Hamady and Yatsunenko117 It is currently believed that such diet-induced changes to the microbial populations in the gut are responsible for the escalating epidemics of chronic illness in the developed world, including obesity Reference Turnbaugh, Hamady and Yatsunenko117,Reference Ley, Turnbaugh, Klein and Gordon118 and inflammatory bowel disease. Reference Devkota, Wang and Musch119 Under these considerations, there are calls to restore the composition, structure, and functioning of the ancestral gut microbiota ecosystem using the concept of “rewilding” (4). Although there are successful examples of rewilding such as the widely celebrated reintroduction of gray wolves (Canis lupus) to Yellowstone National Park; appropriate applications of rewilding remain under debate. For example, Carmody and co-workers Reference Carmody, Sarkar and Reese120 have raised questions about how this could be implemented, considering for example that high microbial plasticity may underpin an industrialized gut microbiota that is reasonably well adapted to its environment, even if it is then less well paired with the host. They proposed that there may be some sort of “third body problem” for the human microbiota environment giving place to an unsolvable puzzle for human health. We think that our Ecosystem Antifragility framework Reference Equihua, Aldama and Gershenson29 and the evidence found here, solve this problem. Taking all into account, using a complex system approach showed that the arrow of health points in the direction of critical/antifragile (more complex) gut microbiota, and that arrow is aligned with non-industrialized lifestyles.

As suggested by Sonnenburg and Sonneburg Reference Sonnenburg and Sonnenburg36 it seems that to fully understand how gut microbiota modulates human health it is necessary to incorporate an ecological perspective to identify gut microbiota ecosystem services. In this way, assessing the impact of an urban industrialized lifestyle on these services might depend on the specifics of numerous factors and could require isolating and archiving bacterial strains that are sensitive to this kind of external perturbations, and conducting specific studies for them. Nevertheless, this traditional approach to ecology based on ecosystem integrity is limited because it has an underlying model for ecosystem health (EH) as a function of the ecosystem state measured as integrity or EH = f(state). But as we have been arguing, we also need to think of the dynamics and how the system responds to perturbation; so for us, it is clear that we need a much wider model of health given by EH = f(state, dynamics, response to perturbations) than the one is given by EH = f(integrity, criticality, antifragility) in terms of assessment. Reference Equihua, Aldama and Gershenson29

Fig. 6 shows a conceptual diagram showing the potential effect of path dependence Reference Jha, Davenport and Gautam77,Reference Jackson, Pawar and Woodward121 that combined with different lifestyles restrict the space of possible network structures and type of response to perturbation. Due to path dependence including lifestyle, gut microbiota ecosystems may turn fragile if they lose complexity under perturbation; robust if it is essentially insensible to it; or antifragile if it benefits from it as has been observed for example in molecular ecological networks in grassland soil microbial communities. Reference Yuan, Guo and Wu122

We consider that this change of framework is not only interesting from the theoretical perspective to understand for example longevity Reference Olivieri, Marchegiani and Matacchione123 but it has also been shown that using its principles of an antifragility perspective may improve clinical practices in oncological drug administration. Reference Taleb and West124

Supplementary material

For supplementary material accompanying this paper visit https://doi.org/10.1017/S2040174423000144

Data Availability Statement

All sequences obtained were uploaded to the NCBI database under the Bioproject number PRJNA593240 with the link: https://www.ncbi.nlm.nih.gov/bioproject/?term=PRJNA593240

Complementary data is available at: =https://osf.io/g6ub2/?view_only=d97583bfc8284db0a294e3233e2b96d0

Acknowledgments

We are grateful to Margarita Muciño, and Julio Naranjo from Xuajin Me’Phaa a non-governmental association, for their help in the liaison with the Me’Phaa community, and their help in sample collection and logistics. We also are grateful to Santiago Martinez-Correa for their contribution to DNA amplification. IG-S explicitly acknowledges the UNAM and PASPA-DGAPA program for the financial support granted to carry out his sabbatical stay and the development of this project.

Conflicts of interest

The authors declare no conflict of interest.

Funding

This project was funded by UNAM-PAPIIT [grant numbers IA209416, IA207019], DGAPA postdoctoral Fellowship, CONACYT Ciencia Básica [grant number 241744], CONACyT Investigadores por México Fellowship.

Institutional review board statement

All procedures for testing, experimental protocols, and recruitment were approved by the National Autonomous University of Mexico Committee on Research Ethics (FPSI/CE/01/2016) and run in accordance with the ethical principles and guidelines of the Official Mexican Law (NOM-012-SSA3-2012).

Informed Consent Statement: All adult participants signed a written informed consent, and for the case of participants under 18 years, we obtained specific written informed consent from their parents, or legal guardians according to the normativity of Mexican Law.

References

Domenico, MD, Brockmann, C, Camargo, CG, et al., Complexity Explained. 2019. DOI 10.17605/OSF.IO/TQGNW.Google Scholar
Gershenson, C, Heylighen, F. When can we call a system self-organizing? In: Advances in Artificial Life, 7th European Conference, ECAL. 2003 LNAI 2801 10.1007/978-3-540-39432-7_65CrossRefGoogle Scholar
Gershenson, C, Fernández, N. Complexity and information: measuring emergence, self-organization, and homeostasis at multiple scales. Complexity. 2012; 18(2), 2944. DOI 10.1002/cplx.20372.CrossRefGoogle Scholar
Huitzil, S, Sandoval-Motta, S, Frank, A, Aldana, M. Modeling the role of the microbiome in evolution. Front Physiol. 2018; 9, 1836. DOI 10.3389/fphys.2018.01836.10.3389/fphys.2018.01836CrossRefGoogle ScholarPubMed
Hidalgo, J, Grilli, J, Suweis, S, et al. Information-based fitness and the emergence of criticality in living systems, Proc Natl Acad Sci U S A, 111, 2014; pp. 1009510100. DOI 10.1073/pnas.1401836111.CrossRefGoogle ScholarPubMed
López-Corona, O, Padilla, P. Fisher information as unifying concept for criticality and antifragility, a primer hypothesis. Res One. 2019. DOI 10.20944/preprints201911.0005.v1.Google Scholar
Goldberger, AL. Fractal mechanisms in the electrophysiology of the heart. IEEE Eng Med Biol Mag. 1992; 11(2), 4752. DOI 10.1109/51.157076.CrossRefGoogle ScholarPubMed
Kiyono, K, Struzik, ZR, Aoyagi, N, Togo, F, Yamamoto, Y. Phase transition in a healthy human heart rate. Phys Rev Lett. 2005; 95(5), 058101. DOI 10.1103/PhysRevLett.95.058101.10.1103/PhysRevLett.95.058101CrossRefGoogle Scholar
Massobrio, P, de Arcangelis, L, Pasquale, V, Jensen, HJ, Plenz, D. Criticality as a signature of healthy neural systems. Front Syst Neurosci. 2015; 9, 22. DOI 10.3389/fnsys.2015.00022.CrossRefGoogle ScholarPubMed
Rivera, AL, González-Montoro, A, Alberola-López, C, et al. Looking for biomarkers in physiological time series. In Quantitative Models for Microscopic to Macroscopic Biological Macromolecules and Tissues, 2018; pp. 111131. Springer. DOI 10.1007/978-3-319-89584-2_5.CrossRefGoogle Scholar
Goldberger, AL, Amaral, LA, Hausdorff, JM, et al. Fractal dynamics in physiology: alterations with disease and aging. Proc Natl Acad Sci U S A. 2002; 99(5), 24662472. DOI 10.1073/pnas.012579499.CrossRefGoogle ScholarPubMed
Schmulevich, I, Dougherty, ER, Kim, S. Gaussian Bayesian networks for inference of signaling pathways and analysis of gene expression data. Bioinformatics. 2005; 21(9), 21152122. DOI 10.1093/bioinformatics/bti282.Google Scholar
Serra, R, Villani, M, Graudenzi, A, Kauffman, S. Why a simple model of genetic regulatory networks describes the distribution of avalanches in gene expression data. J Theor Biol. 2007; 246(3), 449460. DOI 10.1016/j.jtbi.2006.12.036.CrossRefGoogle Scholar
Balleza, E, Alvarez-Buylla, ER, Chaos, A, Kauffman, S, Shmulevich, I. Critical dynamics in genetic regulatory networks: examples from four kingdoms. PLoS One. 2008; 3(6), e2456. DOI 10.1371/journal.pone.0002456.CrossRefGoogle ScholarPubMed
Daniels, BC, Kim, H, Moore, JR, et al. Criticality distinguishes the ensemble of biological regulatory networks. Phys Rev Lett. 2018; 121(13), 138102. DOI 10.1103/PhysRevLett.121.138102.10.1103/PhysRevLett.121.138102CrossRefGoogle ScholarPubMed
Derrida, B, Pomeau, Y. Random networks of automata: a simple annealed approximation. Europhys Lett. 1986; 1(2), 4549. DOI 10.1209/0295-5075/1/2/001.10.1209/0295-5075/1/2/001CrossRefGoogle Scholar
Aldana, M. Boolean dynamics of networks with scale-free topology. Physica D. 2003; 185(1-2), 4566. DOI 10.1016/S0167-2789(02)00749-6.10.1016/S0167-2789(03)00174-XCrossRefGoogle Scholar
Aldana, M, Balleza, E, Kauffman, S, Resendiz, O. Robustness and evolvability in genetic regulatory networks. J Theor Biol. 2007; 245(3), 433448. DOI 10.1016/j.jtbi.2006.10.033.CrossRefGoogle ScholarPubMed
Langton, CG. Computation at the edge of chaos: phase transitions and emergent computation. Physica D. 1990; 42(1-3), 1237. DOI 10.1016/0167-2789(90)90064-V.10.1016/0167-2789(90)90064-VCrossRefGoogle Scholar
Nykter, M, Price, ND, Larjo, A, et al. Critical networks exhibit maximal information diversity in structure-dynamics relationships. Phys Rev Lett. 2008; 100(5), 058702. DOI 10.1103/PhysRevLett.100.058702.CrossRefGoogle ScholarPubMed
Kinouchi, O, Copelli, M. Optimal dynamical range of excitable networks at criticality. Nat Phys. 2006; 2(5), 348351. DOI 10.1038/nphys2897.CrossRefGoogle Scholar
Karimi, B, Maron, PA, Chemidlin-Prevost Boure, N, et al. Microbial diversity and ecological networks as indicators of environmental quality. Environ Chem Lett. 2017; 15(2), 265281. DOI 10.1007/s10311-017-0614-6.10.1007/s10311-017-0614-6CrossRefGoogle Scholar
Banerjee, S, Walder, F, Büchi, L, et al. Agricultural intensification reduces microbial network complexity and the abundance of keystone taxa in roots. ISME J. 2019; 13(7), 17221736. DOI 10.1038/s41396-019-0383-2.CrossRefGoogle ScholarPubMed
Danchin, A, Binder, PM, Noria, S. Antifragility and tinkering in biology (and in business) flexibility provides an efficient epigenetic way to manage risk. Genes-BASEL. 2011; 2(4), 9981016. DOI 10.3390/genes2040998 PMID: 24710068; PMCID: PMC4061651.10.3390/genes2040998CrossRefGoogle ScholarPubMed
Taleb NN. Antifragile: How to live in a world we don't understand. Vol. 3. London: Allen Lane; 2012.Google Scholar
Taleb, NN, Douady, R. Mathematical definition, mapping, and detection of (anti) fragility. Quant Financ. 2013; 13(11), 16771689. DOI 10.1080/14697688.2013.815721.CrossRefGoogle Scholar
Taleb, NN. (anti) fragility and convex responses in medicine. Int Conf Complex Syst. 2018 299325. DOI 10.1007/978-3-319-96661-8_18.Google Scholar
Ramírez-Carrillo, E, López-Corona, O, Toledo-Roy, JC, et al. Assessing sustainability in North America’s ecosystems using criticality and information theory. PloS One. 2018; 13(7), e0200382. DOI 10.1371/journal.pone.0200382.CrossRefGoogle ScholarPubMed
Equihua, M, Aldama, ME, Gershenson, C, et al. Ecosystem antifragility: beyond integrity and resilience. PeerJ. 2020; 8, e8533. DOI 10.7717/peerj.8533.CrossRefGoogle ScholarPubMed
Romano, MC, Jiménez, P, Miranda-Brito, C, Valdez, RA. Parasites and steroid hormones: corticosteroid and sex steroid synthesis, their role in the parasite physiology and development. Front Neurosci. 2015; 9, 224. DOI 10.3389/fnins.2015.00224.CrossRefGoogle ScholarPubMed
Johnson, TP, Nath, A. Neurological syndromes driven by postinfectious processes or unrecognized persistent infections. Curr Opin Neurol. 2018; 31(3), 318324. DOI 10.1097/WCO.0000000000000541.CrossRefGoogle ScholarPubMed
Shepherd, C, Navarro, S, Wangchuk, P, et al. Identifying the immunomodulatory components of helminths. Parasite Immunol. 2015; 37(6), 293303. DOI 10.1111/pim.12186.10.1111/pim.12192CrossRefGoogle ScholarPubMed
Adamo, SA. Modulating the modulators: parasites, neuromodulators and host behavioral change. Brain Behav Evol. 2002; 60(6), 370377. DOI 10.1159/000067719.CrossRefGoogle ScholarPubMed
González-Tokman, D, Córdoba-Aguilar, A, González-Santoyo, I, Lanz-Mendoza, H. Infection effects on feeding and territorial behaviour in a predatory insect in the wild. Anim Behav. 2011; 81(6), 11851194. DOI 10.1016/j.anbehav.2011.02.025.10.1016/j.anbehav.2011.02.027CrossRefGoogle Scholar
Olm, MR, Dahan, D, Carter, MM, et al. Robust variation in infant gut microbiome assembly across a spectrum of lifestyles. Science. 2022; 376(6598), 12201223. DOI 10.1126/science.abm8869.CrossRefGoogle ScholarPubMed
Sonnenburg, JL, Sonnenburg, ED. Vulnerability of the industrialized microbiota. Science. 2019; 366(6464), eaaw9255. DOI 10.1126/science.aaw9255.CrossRefGoogle ScholarPubMed
Rosas-Plaza, S, Hernandez-Teran, A, Navarro-Diaz, M, et al. Human gut microbiome across different lifestyles: from hunter-gatherers to urban populations. Front Microbiol. 2022; 13, 815823. DOI 10.3389/fmicb.2022.815823.CrossRefGoogle ScholarPubMed
Sanchez-Quinto, A, Cerqueda-Garcia, D, Falcon, LI, et al. Gut microbiome in children from indigenous and urban communities in México: different subsistence models, different microbiomes. Microorganisms. 2020; 8(10), 1592. DOI 10.3390/microorganisms8101592.CrossRefGoogle Scholar
Selber-Hnativ, K, Korem, T, Segal, E. Host biomarkers for distinguishing bacterial from non-bacterial causes of acute febrile illness: a comprehensive review. PLoS One. 2017; 12(10), e0189986, 10.1371/journal.pone.0189986, PMID: 29077714; PMCID: PMC5657114.Google Scholar
Ding, RX, Goh, WR, Wu, RN, et al. Revisit gut microbiota and its impact on human health and disease. J Food Drug Anal. 2019; 27(3), 623631. DOI 10.1016/j.jfda.2019.01.002.CrossRefGoogle ScholarPubMed
Ramírez-Carrillo, E, Gaona, O, Nieto, J, et al. Disturbance in human gut microbiota networks by parasites and its implications in the incidence of depression. Sci Rep. 2020; 10(1), 3680. DOI 10.1038/s41598-020-60524-0.doi.CrossRefGoogle ScholarPubMed
Kim, PJ, Price, ND. Genetic co-occurrence network across sequenced microbes. PLoS Comput Biol. 2011; 7(12), e1002340PMID: 22219708; PMCID: PMC324527810.1371/journal.pcbi.1002340.CrossRefGoogle ScholarPubMed
Bassler, BL, Wright, M, Showalter, RE, Silverman, MR. Intercellular signalling in Vibrio harveyi: sequence and function of genes regulating expression of luminescence. Mol Microbiol. 1993; 9(4), 773786. DOI 10.1111/j.1365-2958.1993.tb01737.x.CrossRefGoogle ScholarPubMed
Ackerman, J. The ultimate social network. Sci Am. 2012; 306(6), 3643. DOI 10.1038/scientificamerican0612-36.CrossRefGoogle ScholarPubMed
Williams, SCP. Microbial social networks. HHMI Bull, 2013, 26(3), 16.Google Scholar
Pereira, CS, Thompson, JA, Xavier, KB. AI-2-mediated signalling in bacteria. FEMS Microbiol Rev. 2013; 37(2), 156181. DOI 10.1111/j.1574-6976.2012.00345.x.CrossRefGoogle ScholarPubMed
Fernandez, M, Riveros, JD, Campos, M, Mathee, K, Narasimhan, G. Microbial “social networks”. BMC Genomics. 2015; 16(11), 113. DOI 10.1186/1471-2164-16-S11-S6.CrossRefGoogle ScholarPubMed
Cickovski, T, Peake, E, Aguiar-Pulido, V, Narasimhan, G. ATria: a novel centrality algorithm applied to biological networks. BMC Bioinform. 2017; 18(8), 110. DOI 10.1186/s12859-016-1445-7.CrossRefGoogle Scholar
Atkinson, S, Williams, P. Quorum sensing and social networking in the microbial world. J R Soc Interface. 2009; 6(40), 959978. DOI 10.1098/rsif.2009.0203.10.1098/rsif.2009.0203CrossRefGoogle ScholarPubMed
Jiao, S, Wang, J, Wei, G, Chen, W, Lu, Y. Dominant role of abundant rather than rare bacterial taxa in maintaining agro-soil microbiomes under environmental disturbances. Chemosphere. 2019; 1, 248259. DOI 10.1016/j.chemosphere.2019.05.167.10.1016/j.chemosphere.2019.06.174CrossRefGoogle Scholar
Barragán, A. Gut microbiota and neurogenesis in the enteric nervous system. J Clin Gastroenterol. 2007; 41 Suppl 1, S108S110. DOI 10.1097/MCG.0b013e31815ed49c.Google Scholar
Borda-Niño, M, Hernández-Muciño, D, Ceccon, E. Restauración productiva en la práctica: el caso de las comunidades indígenas me’phaa de la Montaña de Guerrero, México. In Ceccon, E., y Pérez, DR (coordinadores), Más allá de la ecología de la restauración. Perspectivas sociales en América Latina y el Caribe. Buenos Aires: Vázquez Manzzini Editores, 2016, https://www.researchgate.net/profile/Diego-Hernandez-Mucino/publication/309681903_Restauracion_productiva_en_la_practica_el_caso_de_las_comunidades_indigenas_Me_Phaa_de_La_Montana_de_Guerrero_Mexico/links/581d04b608ae40da2cab4244/Restauracion-productiva-en-la-practica-el-caso-de-las-comunidades-indigenas-Me-Phaa-de-La-Montana-de-Guerrero-Mexico.pdf Google Scholar
Black, CA. An autosegmental analysis of Me'phaa (Tlapanec) noun inflection 2004, https://mexico.sil.org/es/resources/archives/2860.Google Scholar
Camacho, Z (Montaña de Guerrero Pobreza y Militarización. Revista Contralínea, 2007. Available online: https://www.contralinea.com.mx/archivo/2007/enero/htm/montana_guerrero_militares.htm.Google Scholar
Miramontes, O, DeSouza, O, Hernández, D, Ceccon, E. Non-Lévy mobility patterns of Mexican Me’Phaa peasants searching for fuel wood. Hum Ecol. 2012; 40, 167174. DOI 10.1007/s10745-011-9443-6.CrossRefGoogle Scholar
Doorduyn, Y, Van Den Brandhof, WE, Van Duynhoven, YTHP, Wannet, WJB, Van Pelt, W. Risk factors for Salmonella Enteritidis and Typhimurium (DT104 and non-DT104) infections in The Netherlands: predominant roles for raw eggs in Enteritidis and sandboxes in Typhimurium infections. Epidemiol Infect. 2006; 134(3), 617626. DOI 10.1017/S095026880500556X, PMID: 16490158; PMCID: PMC2870552.10.1017/S0950268805005406CrossRefGoogle ScholarPubMed
Pavia, AT, Shipman, LD, Wells, JG, et al. Epidemiologic evidence that prior antimicrobial exposure decreases resistance to infection by antimicrobial-sensitive Salmonella. J Infect Dis. 1990; 161(2), 255260. DOI 10.1093/infdis/161.2.255.CrossRefGoogle ScholarPubMed
Stecher, B, Robbiani, R, Walker, AW, et al. Salmonella enterica serovar typhimurium exploits inflammation to compete with the intestinal microbiota. PLoS Biol. 2007; 5(10), e244. DOI 10.1371/journal.pbio.0050244.CrossRefGoogle ScholarPubMed
Hernández-Muciño, D, Borda-Niño, B, Santiago, R, et al. La comunidad me’phaa construye su futuro: agroecología y restauración como herramientas de desarrollo rural sustentable, Experiencias de colaboración transdisciplinaria para la sustentabilidad, 2018. DOI 10.48133/ECOTROPICOS-66-06, 66.Google Scholar
DGIS. Indicadores de salud. In Secretaría de Salud, n.d., http://www.dgis.salud.gob.mx/contenidos/sinais/indica_gral.html.Google Scholar
Lewis, CM, Obregón-Tito, A, Tito, RY, Foster, MW, Spicer, PG. The Human Microbiome Project: lessons from human genomics. Trends Microbiol. 2012; 20(1), 14. DOI 10.1016/j.tim.2011.11.001.CrossRefGoogle ScholarPubMed
Callahan, BJ, McMurdie, PJ, Holmes, SP. Exact sequence variants should replace operational taxonomic units in marker-gene data analysis. ISME J. 2017; 11(12), 26392643. DOI 10.1038/ismej.2017.119.CrossRefGoogle ScholarPubMed
McMurdie, PJ, Holmes, S. phyloseq: an R package for reproducible interactive analysis and graphics of microbiome census data. PLoS One. 2013; 8(4), e61217. DOI 10.1371/journal.pone.0061217.CrossRefGoogle Scholar
NCBI BioProject [Internet] (Bethesda (MD): National Center for Biotechnology Information, 2021). Bioproject Number PRJNA593240. Available at: https://www.ncbi.nlm.nih.gov/bioproject/PRJNA593240/.Google Scholar
Oksanen, J. Cooccur: probabilistic species co-occurrence analysis in R. R package version 1.3.3. Available at: https://CRAN.R-project.org/package=cooccur.Google Scholar
Todd, J. Probiotics and the gut-brain axis: a review. J Clin Gastroenterol. 2005; 39(4), 338346. DOI 10.1097/01.mcg.0000156969.01009.3f.Google Scholar
Bonchev, D, Buck, GA. The role of microbiology and immunology in linking the gut microbiome to human brain function. Neurol Psychiatry Brain Res. 2015; 21(3), 118126. DOI 10.1016/j.npbr.2015.07.003.Google Scholar
Latra-Kivisto, H. Influence of gastrointestinal function on the central nervous system. Int J Circumpolar Health. 2001; 60(4), 575579.Google Scholar
Neel, DL, Orrison, ME. The linear complexity of a graph. In: International Conference on Combinatorial Mathematics and Combinatorial Computing, 2006, Available from: https://scholarship.claremont.edu/hmc_fac_pub/73/.CrossRefGoogle Scholar
Dehmer, M, Emmert-Streib, F, Graber, A, Salvador, A, Shi, Y. A network perspective on microbiome-host interactions: network-based methods to elucidate host-microbiome interactions. Biomed Res Int. 2016; 2016, 12. DOI 10.1155/2016/7851742.Google Scholar
Dehmer, M, Mowshowitz, A. From gut feelings to reasoning: an overview of graphs as a representational framework for biological and biomedical systems. Wiley Interdiscip Rev Comput Stat. 2011; 3(6), 554570. DOI 10.1002/wics.200.Google Scholar
Mowshowitz, A, Dehmer, M. Network approaches to biology. In Handbook of Graphs and Networks, 2012; pp. 345366. DOI 10.1002/9781118165621.ch16.Google Scholar
Cao, S, Dehmer, M, Shi, Y. Extremality of degree-based graph entropies. Inf Sci. 2014; 278, 2233. DOI 10.1016/j.ins.2014.02.096.CrossRefGoogle Scholar
Shannon, P, Markiel, A, Ozier, O, et al. Cytoscape: a software environment for integrated models of biomolecular interaction networks. Genome Res. 2003; 13(11), 24982504. DOI 10.1101/gr.1239303.CrossRefGoogle ScholarPubMed
Ibragimov, R, Malek, M, Guo, J, Baumbach, J. Gedevo: an evolutionary graph edit distance algorithm for biological network alignment. In: German Conference on Bioinformatics 2013. Schloss Dagstuhl-Leibniz-Zentrum fuer Informatik, 2013.Google Scholar
Sánchez-Quinto, A, Cerqueda-García, D, Falcón, LI, et al. Gut microbiome in children from indigenous and urban communities in México: different subsistence models, different microbiomes. Microorganisms. 2020; 8(10), 1592. DOI 10.3390/microorganisms8101592.CrossRefGoogle Scholar
Jha, AR, Davenport, ER, Gautam, Y, et al. Gut microbiome transition across a lifestyle gradient in Himalaya. PLoS Biol. 2018; 16(11), e2005396. DOI 10.1371/journal.pbio.2005396.CrossRefGoogle ScholarPubMed
Segata, N. Gut microbiome: westernization and the disappearance of intestinal diversity. Curr Biol. 2015; 25(14), R611R613. DOI 10.1016/j.cub.2015.05.040.CrossRefGoogle ScholarPubMed
Clemente, JC, Pehrsson, EC, Blaser, MJ, et al. The microbiome of uncontacted Amerindians. Sci Adv. 2015; 1(3), e1500183. DOI 10.1126/sciadv.1500183.CrossRefGoogle ScholarPubMed
Pontzer, H, Raichlen, DA, Wood, BM, et al. Hunter-gatherer energetics and human obesity. PLoS One. 2012; 7(7), e40503. DOI 10.1371/journal.pone.0040503.CrossRefGoogle ScholarPubMed
Anwesh, M, Kumar, KV, Nagarajan, M, et al. Elucidating the richness of bacterial groups in the gut of Nicobarese Tribal Community—perspective on their lifestyle transition. Anaerobe. 2016; 39, 6876. DOI 10.1016/j.anaerobe.2016.03.005.CrossRefGoogle ScholarPubMed
Martínez, I, Stegen, JC, Maldonado-Gomez, MX, et al. The gut microbiota of rural papua new guineans: composition, diversity patterns, and ecological processes. Cell Rep. 2015; 11(4), 527538. DOI 10.1016/j.celrep.2015.03.049.CrossRefGoogle ScholarPubMed
Kaplan, H, Huttenhower, C, Pearce, D, Godfrey, KM. The gut-brain axis, human microbiota and behavior. Nat Rev Microbiol. 2019; 17(8), 383396. DOI 10.1038/s41579-019-0229-6.Google Scholar
Arumugam, M, Raes, J, Pelletier, E, et al. Enterotypes of the human gut microbiome. Nature. 2011; 473(7346), 174180. DOI 10.1038/nature09944.CrossRefGoogle ScholarPubMed
Roswell, M, Dushoff, J, Winfree, R. A conceptual guide to measuring species diversity. Oikos. 2021; 130(3), 321328. DOI 10.1111/oik.08087.CrossRefGoogle Scholar
Konopiński, MK. Shannon diversity index: a call to replace the original Shannon’s formula with unbiased estimator in the population genetics studies. PeerJ. 2020; 8, e9391. DOI 10.7717/peerj.9391.CrossRefGoogle Scholar
Ramírez-Carrillo, E, G-Santoyo, I, López-Corona, O, et al. Similar connectivity of gut microbiota and brain activity networks is mediated by animal protein and lipid intake in children from a Mexican indigenous population. PLoS One, Accepted for publication,Google Scholar
Van Dellen, E, Douw, L, Hillebrand, A, et al. Epilepsy surgery outcome and functional network alterations in longitudinal MEG: a minimum spanning tree analysis. Neuroimage. 2014; 86, 354363. DOI 10.1016/j.neuroimage.2013.09.058.CrossRefGoogle ScholarPubMed
Cohen, R, Havlin, S. Scaling properties of complex networks and spanning trees. In Handbook of Large-scale Random Networks, 2008; pp. 143169. DOI 10.1007/978-0-387-77669-0_6.CrossRefGoogle Scholar
van Dellen, E, Sommer, IE, Bohlken, MM, et al. Minimum spanning tree analysis of the human connectome. Hum Brain Mapp. 2018; 39(6), 24552471. DOI 10.1002/hbm.24030.CrossRefGoogle ScholarPubMed
Stam, CJ, Tewarie, P, Van Dellen, E, et al. The trees and the forest: characterization of complex brain networks with minimum spanning trees. Int J Psychophysiol. 2014; 92(3), 129138. DOI 10.1016/j.ijpsycho.2014.05.004.CrossRefGoogle ScholarPubMed
Van Mieghem, P, van Langen, S. Influence of the link weight structure on the shortest path. Phys Rev E. 2005; 71(5), 056113. DOI 10.1103/PhysRevE.71.056113.CrossRefGoogle ScholarPubMed
Saba, V, Premi, E, Cristillo, V, et al. Brain connectivity and information-flow breakdown revealed by a minimum spanning tree-based analysis of MRI data in behavioral variant frontotemporal dementia. Front Neurosci. 2019; 13, 211. DOI 10.3389/fnins.2019.00211.CrossRefGoogle ScholarPubMed
Vourkas, M, Karakonstantaki, E, Simos, PG, et al. Simple and difficult mathematics in children: a minimum spanning tree EEG network analysis. Neurosci Lett. 2014; 10, 2833. DOI 10.1016/j.neulet.2014.05.029.CrossRefGoogle Scholar
González, GF, Van der Molen, MJW, Žarić, G, et al. Graph analysis of EEG resting state functional networks in dyslexic readers. Clin Neurophysiol. 2016; 127(9), 31653175. DOI 10.1016/j.clinph.2016.05.009.CrossRefGoogle Scholar
Fraschini, M, Demuru, M, Hillebrand, A, et al. EEG functional network topology is associated with disability in patients with amyotrophic lateral sclerosis. Sci Rep. 2016; 6(1), 38653. DOI 10.1038/srep38653.CrossRefGoogle ScholarPubMed
Crobe, A, Demuru, M, Didaci, L, Marcialis, GL, Fraschini, M. Minimum spanning tree and k-core decomposition as measure of subject-specific EEG traits. Biomed Phys Eng Express. 2016; 2(1), 017001. DOI 10.1088/2057-1976/2/1/017001.CrossRefGoogle Scholar
Demuru, M, Fara, F, Fraschini, M. Brain network analysis of EEG functional connectivity during imagery hand movements. J Integr Neurosci. 2013; 12(4), 441447. DOI 10.1142/S0219635213500284.CrossRefGoogle ScholarPubMed
Dauwan, M, Van Dellen, E, van Boxtel, L, et al. EEG-directed connectivity from posterior brain regions is decreased in dementia with Lewy bodies: a comparison with Alzheimer’s disease and controls. Neurobiol Aging. 2016; 41, 122129. DOI 10.1016/j.neurobiolaging.2016.02.010.CrossRefGoogle ScholarPubMed
López-Corona, O, Kolb, M, Ramírez-Carrillo, E, Lovett, J. ESD ideas: planetary antifragility: a new dimension in the definition of the safe operating space for humanity. Earth Syst Dynam. 2022; 13(3), 11451155. DOI 10.5194/esd-13-1145-2022.CrossRefGoogle Scholar
Packard, NH. Adaptation toward the edge of chaos. Dyn Patterns Complex Syst. 1988; 212, 293301. DOI 10.1007/978-1-4612-3784-6_29.Google Scholar
Langton, CG. Computation at the edge of chaos: phase transitions and emergent computation. Phys D Nonlinear Phenomena. 1990; 42(1-3), 1237. DOI 10.1016/0167-2789(90)90064-V.CrossRefGoogle Scholar
Langton, CG. Life at the edge of chaos. In Artificial Life II. Santa Fe Institute Studies in the Science of Complexity.1992, ISBN: 978-0201525715,Google Scholar
Kauffman, SA. The origins of order: Self-organization and selection in evolution, 1993. Oxford University Press, USA.ISBN: 978-0195079517,Google Scholar
Kauffman, S, Kauffman, SA. At home in the universe: the search for laws of self-organization and complexity 1995). USA;: Oxford University Press, ISBN: 0195095995.Google Scholar
Benedettini, S, Villani, M, Roli, A, et al. Dynamical regimes and learning properties of evolved Boolean networks. Neurocomputing. 2013; 99, 111123. DOI 10.1016/j.neucom.2012.03.002.CrossRefGoogle Scholar
Coyte, KZ, Schluter, J, Foster, KR. The ecology of the microbiome: networks, competition, and stability. Science. 2015; 350(6260), 663666. DOI 10.1126/science.aad2602.CrossRefGoogle ScholarPubMed
Layeghifard, M, Hwang, DM, Guttman, DS. Disentangling interactions in the microbiome: a network perspective. Trends Microbiol. 2017; 25(3), 217228. DOI 10.1016/j.tim.2016.11.008.CrossRefGoogle ScholarPubMed
Smits, SA, Leach, J, Sonnenburg, ED, et al. Seasonal cycling in the gut microbiome of the Hadza hunter-gatherers of Tanzania. Science. 2017; 357(6353), 802806. DOI 10.1126/science.aan4834.CrossRefGoogle ScholarPubMed
De Filippo, C, Cavalieri, D, Di Paola, M, et al. Impact of diet in shaping gut microbiota revealed by a comparative study in children from Europe and rural Africa. Proc Natl Acad Sci U S A. 2010; 107(33), 1469114696. DOI 10.1073/pnas.1005963107.CrossRefGoogle ScholarPubMed
Yatsunenko, T, Rey, FE, Manary, MJ, et al. Human gut microbiome viewed across age and geography. Nature. 2012; 486(7402), 222227. DOI 10.1038/nature11053.CrossRefGoogle ScholarPubMed
Obregon-Tito, AJ, Tito, RY, Metcalf, J, et al. Subsistence strategies in traditional societies distinguish gut microbiomes. Nat Commun. 2015; 6(1), 6505. DOI 10.1038/ncomms7505.CrossRefGoogle ScholarPubMed
Angelakis, E, Yasir, M, Bachar, D, et al. Gut microbiome and dietary patterns in different Saudi populations and monkeys. Sci Rep. 2016; 6(1), 26814. DOI 10.1038/srep26814.CrossRefGoogle ScholarPubMed
Tett, A, Huang, KD, Asnicar, F, et al. The Prevotella copri complex comprises four distinct clades underrepresented in westernized populations. Cell Host Microbe. 2019; 26(5), 666679. DOI 10.1016/j.chom.2019.09.007.CrossRefGoogle ScholarPubMed
Sandoval-Motta, S, Aldana, M, Frank, A. Evolving ecosystems: inheritance and selection in the light of the microbiome. Arch Med Res. 2017; 48(8), 780789. DOI 10.1016/j.arcmed.2017.12.007.CrossRefGoogle ScholarPubMed
Wibowo, MC, Yang, Z, Borry, M, et al. Reconstruction of ancient microbial genomes from the human gut. Nature. 2021; 594(7862), 234239. DOI 10.1038/s41586-021-03578-9.CrossRefGoogle ScholarPubMed
Turnbaugh, PJ, Hamady, M, Yatsunenko, T, et al. A core gut microbiome in obese and lean twins. Nature. 2009; 457(7228), 480484. DOI 10.1038/nature07540.CrossRefGoogle ScholarPubMed
Ley, RE, Turnbaugh, PJ, Klein, S, Gordon, JI. Human gut microbes associated with obesity. Nature. 2006; 444(7122), 10221023. DOI 10.1038/4441022a.CrossRefGoogle ScholarPubMed
Devkota, S, Wang, Y, Musch, MW, et al. Dietary-fat-induced taurocholic acid promotes pathobiont expansion and colitis in Il10−/− mice. Nature. 2012; 487(7405), 104108. DOI 10.1038/nature11225.CrossRefGoogle ScholarPubMed
Carmody, RN, Sarkar, A, Reese, AT, et al. Gut microbiota through an evolutionary lens. Science. 2021; 372(6541), 462463. DOI 10.1126/science.abg1629.CrossRefGoogle ScholarPubMed
Jackson, MC, Pawar, S, Woodward, G. The temporal dynamics of multiple stressor effects: from individuals to ecosystems. Trends Ecol Evol. 2021; 36(5), 402410. DOI 10.1016/j.tree.2021.02.010.CrossRefGoogle ScholarPubMed
Yuan, MM, Guo, X, Wu, L, et al. Climate warming enhances microbial network complexity and stability. Nat Clim Chang. 2021; 11(4), 343348. DOI 10.1038/s41558-021-01000-4.CrossRefGoogle Scholar
Olivieri, F, Marchegiani, F, Matacchione, G, et al. Sex/gender-related differences in inflammaging. Mech Ageing Dev. 2023, 111792. DOI 10.1016/j.mad.2023.111792.CrossRefGoogle ScholarPubMed
Taleb, NN, West, J. Working with convex responses: antifragility from finance to oncology. Entropy. 2023; 25(2), 343. DOI 10.3390/e25020343.CrossRefGoogle ScholarPubMed
Figure 0

Figure 1. Locations of Plan de Gatica and El Naranjo, indigenous localities located in the municipality of Ayutla de los Libres and Acatepec (respectively) in the Montaña Alta region of the state of Guerrero, México. Families of these locations were the study subject of this research.

Figure 1

Figure 2. We show the GED analysis score of gut microbiota ecosystem network for the Rural-NP group (considered as the control group for comparison) and the two under perturbation (Rural-P, Urban NP).

Figure 2

Figure 3. Network metrics usually associated with connectivity for the three populations.

Figure 3

Figure 4. Complementary network measurements metrics.

Figure 4

Figure 5. Difference of Shannon Information (emergence) for the three populations (W = 162, p-value = 0.037). The box plot shows the median, quartiles, min-max, and point is the mean.

Figure 5

Figure 6. Conceptual figure showing the effect of path dependence on the set of possible future configurations for gut microbiota ecosystem in terms of how it responds to perturbations to complexity as a general payoff function valid for systems under eco-evolutionary processes, and that define three types of configurations: fragility when it responds in a nonlinear concave way; robust if it is essentially insensible to perturbations or antifragile if it responds in a nonlinear convex way.

Supplementary material: File

G-Santoyo et al. supplementary material

G-Santoyo et al. supplementary material

Download G-Santoyo et al. supplementary material(File)
File 1.1 MB