The traditional approach in medicine is to define diseases phenotypically based on clinically demonstrable signs and symptoms. When our understanding of the nervous system was embryonic, neurological and psychiatric conditions were considered to have the same origin as they commonly co-occur, leading to the historical association of these specialities.
Reference Price, Adams and Coyle1
As our appreciation for differences in conditions affecting the central nervous system (CNS) increased, the study of “organic diseases” of the nervous system became strictly separated from mental illness. Advances in genetics and neurobiology have shed new light on almost all conditions that affect the CNS. They have provided the basis for attempts at biological treatments, leading to these specialities edging closer to each other. Whether neurology and psychiatry should re-merge is a matter of debate. Notably, newly identified disease markers could lead to novel definitions of neurological and psychiatric conditions based on their pathophysiological underpinnings rather than phenotype and symptomatology.
Despite this increased understanding of pathophysiological processes, we continue to divide diseases into phenotypic categories: mood disorders, movement disorders, epilepsy and cerebrovascular disease, amongst others. This approach has been largely successful due to the fortuitously close association between phenotype and pathophysiology. It is most often pathophysiology that determines, for instance, whether a treatment is efficacious or not. Recognising a migraine headache as distinct from an epileptic seizure allows neurologists to consider prescribing a triptan rather than an antiseizure medication. This symptomatic approach, unfortunately, is fallible. The symptoms are similar but treating a migrainous visual aura will not be like treating an epileptic visual hallucination.
The future of neurology and psychiatry will be different. Our growing understanding of complex disease mechanisms allows diseases to be defined by their multi-factorial pathophysiological underpinnings rather than phenotype and symptomatology. There are recent attempts, for example, to reorient the scientific community to a biological definition of Alzheimer’s disease based on biomarkers of neuropathological changes attacking the individual rather than on the clinical manifestations they may (or may not) manifest.
Reference Dubois, Feldman and Jacova2
The new classification of epilepsy is founded on the concept of potentially overlapping aetiologies which only together produce the final epilepsy syndrome.
Reference Scheffer, Berkovic and Capovilla3
We propose that the neuroscience community continue this move beyond pure symptomatic classification schemes towards pathophysiological classifications for all CNS disorders, including psychiatric conditions.
We propose that neurological and psychiatric diseases can be divided into seven interacting pathophysiological spectra: degenerative, functional, structural-connective, infectious, metabolic, toxic/nutritional deficiency and immune/inflammatory (Table 1 and Figure 1a). We have chosen to use the term spectra to emphasise that these categories exist in gradations between individuals. In addition, they are not mutually exclusive, and a single disease or process may belong to several ranges. Cerebral trauma, for example, is an interaction between structural (from the cerebral contusion) and inflammatory processes.
Reference Woodcock and Morganti-Kossmann4
This potential to interact is critical, as one spectrum’s presence and gradation likely influences others at play in an individual. Such complex system interactions are increasingly emerging as central to all areas of biology and medicine.
Figure 1: (A) The pathophysiological spectra for neurological diseases. (B) The modification systems that affect the neurological state of an individual.
Table 1: Definitions of pathophysiological spectra
Understanding the pathophysiological spectra involved in neurological or psychiatric disease, however, is insufficient to entirely understand why the same condition results in different clinical manifestations in other individuals. Such an understanding requires moving beyond a disease-oriented focus toward a systems approach. The CNS responds to injury or disease activators differently depending on their interactions with other factors. Complex system interactions emphasise a move away from the individual organism, organ, molecule, gene or disease. They instead focus on how different entities interact with each other and their environment to result in the final system function (or dysfunction).
Reference De Haan5
Systems approaches emphasise that various factors can mutually influence each other in feedback loops instead of simplistic mono-linear cause–effect relationships. To understand complex diseases, successful collaborations with multiple disciplines in systems biology, using informatics and mathematical models informed by philosophy, will allow us to understand molecular pathways and circular feedback loops and the clinical presentation in a person and the population. This would align with other contemporary attempts, notably in psychiatry, to develop further the Biopsychosocial model introduced in the 1970s, to account for complex feedback loops, learning and plasticity.
Reference De Haan5,Reference Kirmayer and Gómez-Carrillo6
We propose that these factors working outside of the interacting spectra be referred to as modifiers (Figure 1b). These are the mechanisms determining the clinical presentation in an individual and “system”, given the potential for myriad and complex interactions between these systems and the pathophysiological spectra. We propose that these modifiers be divided into the individual’s genome and methylation status, the stage of nervous system development, the internal environment (proteomics, metabolomics and other ∼omics, but also psychological factors) and the external environment (including social and biological factors such as pollution and global warming).
The interplay between spectra and modifiers will determine the disorder’s characteristics in an individual. Hippocampal malrotation, for example, is a congenital malformation generally asymptomatic; however, it increases the risk of febrile status epilepticus in some young individuals.
Reference Shinnar, Bello and Chan7
It has been suggested to increase the subsequent risk of hippocampal sclerosis and mesial temporal lobe epilepsy. Epigenetic changes modify gene expression through DNA methylation, histone modifications and microRNA regulation.
Reference Cacabelos8
Epigenetic changes are a clear means for the external environment to influence the phenotypical expression of the genome. They can explain symptomatic differences between individuals in response to their environment and changes in phenotype in the same individual with increasing age. Multiple sclerosis starts as an inflammatory disease, but there is evidence of genetic risk factors, in particular variants within the human leukocyte antigen complex and that these interact with environmental stimuli such as Epstein Barr virus exposure, smoking and adolescent obesity.
Reference Olsson, Barcellos and Alfredsson9
Advances in understanding the human CNS allow for increasingly pathophysiology-based organisations and classifications of neurological and psychiatric diseases. Going beyond this, we propose that systems relevant approaches will deepen this understanding. We present a view where the complex interactions between pathophysiological spectra and modifiers (including general physical and mental health and the environment) are needed to understand the disease state of an individual. An emphasis on the biological-systemic underpinnings of illness will allow for more refined hypotheses regarding targeted interventions. Other areas of medicine are moving toward personalised approaches, tailoring treatment and interventions to the individual, thus improving care and increasing the chances for cure. We are hopeful that a biological-systemic approach will also encourage personalised care in neurology and psychiatry.
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The traditional approach in medicine is to define diseases phenotypically based on clinically demonstrable signs and symptoms. When our understanding of the nervous system was embryonic, neurological and psychiatric conditions were considered to have the same origin as they commonly co-occur, leading to the historical association of these specialities. Reference Price, Adams and Coyle1 As our appreciation for differences in conditions affecting the central nervous system (CNS) increased, the study of “organic diseases” of the nervous system became strictly separated from mental illness. Advances in genetics and neurobiology have shed new light on almost all conditions that affect the CNS. They have provided the basis for attempts at biological treatments, leading to these specialities edging closer to each other. Whether neurology and psychiatry should re-merge is a matter of debate. Notably, newly identified disease markers could lead to novel definitions of neurological and psychiatric conditions based on their pathophysiological underpinnings rather than phenotype and symptomatology.
Despite this increased understanding of pathophysiological processes, we continue to divide diseases into phenotypic categories: mood disorders, movement disorders, epilepsy and cerebrovascular disease, amongst others. This approach has been largely successful due to the fortuitously close association between phenotype and pathophysiology. It is most often pathophysiology that determines, for instance, whether a treatment is efficacious or not. Recognising a migraine headache as distinct from an epileptic seizure allows neurologists to consider prescribing a triptan rather than an antiseizure medication. This symptomatic approach, unfortunately, is fallible. The symptoms are similar but treating a migrainous visual aura will not be like treating an epileptic visual hallucination.
The future of neurology and psychiatry will be different. Our growing understanding of complex disease mechanisms allows diseases to be defined by their multi-factorial pathophysiological underpinnings rather than phenotype and symptomatology. There are recent attempts, for example, to reorient the scientific community to a biological definition of Alzheimer’s disease based on biomarkers of neuropathological changes attacking the individual rather than on the clinical manifestations they may (or may not) manifest. Reference Dubois, Feldman and Jacova2 The new classification of epilepsy is founded on the concept of potentially overlapping aetiologies which only together produce the final epilepsy syndrome. Reference Scheffer, Berkovic and Capovilla3 We propose that the neuroscience community continue this move beyond pure symptomatic classification schemes towards pathophysiological classifications for all CNS disorders, including psychiatric conditions.
We propose that neurological and psychiatric diseases can be divided into seven interacting pathophysiological spectra: degenerative, functional, structural-connective, infectious, metabolic, toxic/nutritional deficiency and immune/inflammatory (Table 1 and Figure 1a). We have chosen to use the term spectra to emphasise that these categories exist in gradations between individuals. In addition, they are not mutually exclusive, and a single disease or process may belong to several ranges. Cerebral trauma, for example, is an interaction between structural (from the cerebral contusion) and inflammatory processes. Reference Woodcock and Morganti-Kossmann4 This potential to interact is critical, as one spectrum’s presence and gradation likely influences others at play in an individual. Such complex system interactions are increasingly emerging as central to all areas of biology and medicine.
Figure 1: (A) The pathophysiological spectra for neurological diseases. (B) The modification systems that affect the neurological state of an individual.
Table 1: Definitions of pathophysiological spectra
Understanding the pathophysiological spectra involved in neurological or psychiatric disease, however, is insufficient to entirely understand why the same condition results in different clinical manifestations in other individuals. Such an understanding requires moving beyond a disease-oriented focus toward a systems approach. The CNS responds to injury or disease activators differently depending on their interactions with other factors. Complex system interactions emphasise a move away from the individual organism, organ, molecule, gene or disease. They instead focus on how different entities interact with each other and their environment to result in the final system function (or dysfunction). Reference De Haan5 Systems approaches emphasise that various factors can mutually influence each other in feedback loops instead of simplistic mono-linear cause–effect relationships. To understand complex diseases, successful collaborations with multiple disciplines in systems biology, using informatics and mathematical models informed by philosophy, will allow us to understand molecular pathways and circular feedback loops and the clinical presentation in a person and the population. This would align with other contemporary attempts, notably in psychiatry, to develop further the Biopsychosocial model introduced in the 1970s, to account for complex feedback loops, learning and plasticity. Reference De Haan5,Reference Kirmayer and Gómez-Carrillo6
We propose that these factors working outside of the interacting spectra be referred to as modifiers (Figure 1b). These are the mechanisms determining the clinical presentation in an individual and “system”, given the potential for myriad and complex interactions between these systems and the pathophysiological spectra. We propose that these modifiers be divided into the individual’s genome and methylation status, the stage of nervous system development, the internal environment (proteomics, metabolomics and other ∼omics, but also psychological factors) and the external environment (including social and biological factors such as pollution and global warming).
The interplay between spectra and modifiers will determine the disorder’s characteristics in an individual. Hippocampal malrotation, for example, is a congenital malformation generally asymptomatic; however, it increases the risk of febrile status epilepticus in some young individuals. Reference Shinnar, Bello and Chan7 It has been suggested to increase the subsequent risk of hippocampal sclerosis and mesial temporal lobe epilepsy. Epigenetic changes modify gene expression through DNA methylation, histone modifications and microRNA regulation. Reference Cacabelos8 Epigenetic changes are a clear means for the external environment to influence the phenotypical expression of the genome. They can explain symptomatic differences between individuals in response to their environment and changes in phenotype in the same individual with increasing age. Multiple sclerosis starts as an inflammatory disease, but there is evidence of genetic risk factors, in particular variants within the human leukocyte antigen complex and that these interact with environmental stimuli such as Epstein Barr virus exposure, smoking and adolescent obesity. Reference Olsson, Barcellos and Alfredsson9
Advances in understanding the human CNS allow for increasingly pathophysiology-based organisations and classifications of neurological and psychiatric diseases. Going beyond this, we propose that systems relevant approaches will deepen this understanding. We present a view where the complex interactions between pathophysiological spectra and modifiers (including general physical and mental health and the environment) are needed to understand the disease state of an individual. An emphasis on the biological-systemic underpinnings of illness will allow for more refined hypotheses regarding targeted interventions. Other areas of medicine are moving toward personalised approaches, tailoring treatment and interventions to the individual, thus improving care and increasing the chances for cure. We are hopeful that a biological-systemic approach will also encourage personalised care in neurology and psychiatry.
Funding
JWS is based at NIHR University College London Hospitals Biomedical Research Centre, which receives a proportion of funding from the UK Department of Health. He receives research support from the Dr Marvin Weil Epilepsy Research Fund, the Christelijke Verenigingvoor de Verpleging van Lijdersaan Epilepsie, Netherlands, and the UK Epilepsy Society.
Disclosures
M. R. K. reports unrestricted educational grants from Jazz Pharmaceuticals, Eisai, and UCB; and research grants for investigator-initiated studies from Eisai and UCB. J.W.S. reports fees as speaker or consultant from Eisai, UCB, GW Pharmaceuticals, Angelini and Zogenix. P.R.B. reports no competing interests.
Statement of authorship
The authors of this paper have each contributed to the ideas and writing that form the manuscript concerning their respective skills, knowledge and expertise. All authors reviewed the manuscript throughout its production and agreed on the final version.