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Plant protein, fibre and physical activity solutions to address poor appetite and prevent undernutrition in older adults: study protocol for the APPETITE randomised controlled trial

Published online by Cambridge University Press:  10 October 2024

Katy M. Horner*
Affiliation:
School of Public Health, Physiotherapy and Sport Science, University College Dublin, Dublin 4, Republic of Ireland Institute for Food and Health, University College Dublin, Dublin 4, Republic of Ireland Institute for Sport and Health, University College Dublin, Dublin 4, Republic of Ireland
Brian Mullen
Affiliation:
School of Public Health, Physiotherapy and Sport Science, University College Dublin, Dublin 4, Republic of Ireland Institute for Food and Health, University College Dublin, Dublin 4, Republic of Ireland Institute for Sport and Health, University College Dublin, Dublin 4, Republic of Ireland
Anna Quinn
Affiliation:
School of Public Health, Physiotherapy and Sport Science, University College Dublin, Dublin 4, Republic of Ireland Institute for Food and Health, University College Dublin, Dublin 4, Republic of Ireland Institute for Sport and Health, University College Dublin, Dublin 4, Republic of Ireland
Pia Scheufele
Affiliation:
Institute for Biomedicine of Aging, Friedrich-Alexander-Universität Erlangen-Nürnberg, Nuremberg, Germany
Susanne Gola
Affiliation:
Fraunhofer Institute for Process Engineering and Packaging, Freising, Germany
Federica Gonnelli
Affiliation:
Department of Biomedical Sciences, University of Padova, Padova, Italy
Matteo Bozzato
Affiliation:
Department of Biomedical Sciences, University of Padova, Padova, Italy
Jedd Pratt
Affiliation:
Department of Biomedical Sciences, University of Padova, Padova, Italy Department of Sport and Exercise Sciences, Manchester Metropolitan University Institute of Sport, Manchester, UK
Wiktoria Sala
Affiliation:
School of Public Health, Physiotherapy and Sport Science, University College Dublin, Dublin 4, Republic of Ireland
Sinead Mullin
Affiliation:
School of Public Health, Physiotherapy and Sport Science, University College Dublin, Dublin 4, Republic of Ireland
Laura Kirwan
Affiliation:
School of Public Health, Physiotherapy and Sport Science, University College Dublin, Dublin 4, Republic of Ireland
Dominique Dardevet
Affiliation:
Université Clermont Auvergne, INRAE, UNH, Clermont-Ferrand, France
Christelle Guillet
Affiliation:
Université Clermont Auvergne, INRAE, UNH, Clermont-Ferrand, France
Giuseppe De Vito
Affiliation:
Department of Biomedical Sciences, University of Padova, Padova, Italy
Marjolein Visser
Affiliation:
Department of Health Sciences, Faculty of Science, and the Amsterdam Public Health Research Institute, Vrije Universiteit Amsterdam, Amsterdam, The Netherlands
Dorothee Volkert
Affiliation:
Institute for Biomedicine of Aging, Friedrich-Alexander-Universität Erlangen-Nürnberg, Nuremberg, Germany
Clare A. Corish
Affiliation:
School of Public Health, Physiotherapy and Sport Science, University College Dublin, Dublin 4, Republic of Ireland Institute for Food and Health, University College Dublin, Dublin 4, Republic of Ireland
*
*Corresponding author: Dr Katy Horner, email katy.horner@ucd.ie
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Abstract

Reduced appetite with ageing is a key factor that may increase risk of undernutrition. The objective of this study is to determine the impact of innovative plant protein fibre (PPF) products within a personalised optimised diet (PD), a physical activity (PA) programme, and their combination on appetite, and other nutritional, functional and clinical outcomes in community-dwelling older adults in a multi-country randomised controlled intervention trial. One hundred and eighty community-dwelling adults (approximately sixty per trial centre in Germany, Ireland and Italy) aged 65 years and over will be recruited to participate in a 12-week, parallel-group, controlled trial. Participants will be randomised into one of four groups: 1, PD (incorporating two PPF products): 2, PA; 3, PD + PA; and 4, no intervention (control). The primary outcome is appetite measured by visual analogue scales and energy intake from an ad libitum test meal. Secondary outcomes include fasting and postprandial appetite-related gut hormones, Simplified Nutritional Appetite Questionnaire score, body composition, cardiorespiratory fitness, muscle strength, physical function and PA. In addition, self-efficacy, cognitive status, dietary restraint, depressive symptoms and compliance and acceptability of the intervention will be assessed. Metabolomic profiles, RMR, muscle motor unit properties and gut microbiome will also be assessed to explore potential underlying mechanisms. This multi-centre randomised controlled trial will advance knowledge on how PD (incorporating PPF products), PA and their combination influence appetite, nutritional status and related health outcomes in community-dwelling older adults and contribute to the prevention of undernutrition. Trial registration: Clinical Trials.gov Registry NCT05608707 (registered on 2 November 2022). Protocol Version: NCT05608707 Version 4 (registered on 29 September 2023).

Type
Protocol Paper
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), 2024. Published by Cambridge University Press on behalf of The Nutrition Society

Older adults are at high risk of poor appetite and undernutrition, which can lead to frailty, sarcopenia and poor health outcomes(Reference Roberts, Lim and Cox1Reference Volkert, Kiesswetter and Cederholm7). Although definitions of appetite vary(Reference Blundell, De Graaf and Hulshof8), reduced appetite and food intake occurs even in healthy older adults and manifests alongside reductions in muscle mass(Reference Morley3,Reference Morley6,Reference Soenen and Chapman9,Reference Giezenaar, Chapman and Luscombe-Marsh10) . A meta-analysis of fifty-nine studies comparing healthy older with younger adults reported hunger to be 25 % (fasting) to 39 % (postprandial) lower and energy intake to be 16–20 % lower in the older adults(Reference Giezenaar, Chapman and Luscombe-Marsh10).

Multiple environmental, psychological and physiological factors are implicated in appetite deterioration in older adults. For example, social isolation, depression, loss of pleasure in food and taste decline all contribute to reduced appetite(Reference Malafarina, Uriz-Otano and Gil-Guerrero11Reference Fluitman, Hesp and Kaihatu13). Physiological factors include altered gut and other peripheral hormones related to appetite, reduced gut motility, inflammation and changes in the central control of food intake(Reference Malafarina, Uriz-Otano and Gil-Guerrero11,Reference Franceschi, Capri and Monti14) . Reduced fat-free mass and resting energy expenditure and an altered gut microbiome have also been implicated as determinants of reduced appetite in older adults(Reference Cox, Morrison and Ibrahim12,Reference de Souto Barreto and Cesari15,Reference Cox, Bowyer and Ni Lochlainn16) , although evidence of causal associations is currently limited. Multicomponent intervention strategies are therefore needed to address appetite decline and prevent undernutrition(Reference Volkert, Beck and Cederholm2,Reference Cox, Morrison and Ibrahim12) .

The need for interventions to address reduced appetite in older adults, or to increase dietary intake despite a reduced appetite, has been clearly recognised and should be a key target for reducing nutrient deficiencies and risk of undernutrition(Reference de Souto Barreto and Cesari15,Reference Fielding, Landi and Smoyer17) . However, current pharmacological interventions have limited utility in clinical practice(Reference de Souto Barreto and Cesari15). Appropriate nutrition and exercise are considered the optimal strategies to limit declines in muscle mass and function with ageing(Reference Bauer, Biolo and Cederholm18,Reference Deutz, Bauer and Barazzoni19) . Adequate protein and dietary fibre intakes are essential for healthy ageing. Adequate protein intake is important to reduce age-related declines in muscle mass, strength and function(Reference Murphy, Oikawa and Phillips20,Reference Mendonça, Hengeveld and Visser21) . Adequate fibre intake is associated with normal bowel function, reduced intestinal transit times and reduced risk of several non-communicable diseases, among other health benefits(Reference McKeown, Fahey and Slavin2224). For older adults, daily consumption of at least 1·0–1·2 g/kg body weight of protein(Reference Bauer, Biolo and Cederholm18,Reference Deutz, Bauer and Barazzoni19) and 25–30 g of fibre(24,25) is recommended. However, intakes of both nutrients are often sub-optimal in European older adults(23,Reference Kehoe, Walton and Flynn26Reference Stephen, Champ and Cloran31) , including in those with poor appetite(Reference Van Der Meij, Wijnhoven and Lee27). In a cross-sectional analysis of over 2500 community-dwelling older adults, those with a poor appetite were found to have a lower intake of protein and dietary fibre compared with those with good appetite, after adjustment for energy intake and other potential confounders(Reference Van Der Meij, Wijnhoven and Lee27).

With regard to effects on appetite and energy intake, a systematic review of acute and longitudinal studies found protein supplementation (through supplements or whole foods) has no negative impact on overall energy intake in older adults(Reference Ben-Harchache, Roche and Corish32). Similarly, a systematic review of thirty-eight different fibre sources found most isolated fibres did not acutely suppress appetite or energy intake in the general population and a recent 10-week intervention in older adults demonstrated pea hull fibre (10 g/d) supplementation did not suppress appetite(Reference Clark and Slavin33,Reference Alyousif, Mendoza and Auger34) . Interestingly, older adults with poor appetite also appear to have a preference towards non-dairy and high-fibre foods(Reference Van Der Meij, Wijnhoven and Finlayson35). Therefore, addition of plant protein and fibre to the habitual diet appears a promising strategy to improve intake of these nutrients and enhance related health outcomes. Both nutrients may impact several mechanisms implicated in appetite decline with ageing such as alterations in gut motility, inflammation, fat-free mass and the gut microbiome and metabolite profiles(Reference Malafarina, Uriz-Otano and Gil-Guerrero11,Reference Franceschi, Capri and Monti14,Reference Cox, Bowyer and Ni Lochlainn16,24,Reference Johnson, Holliday and Mistry36Reference Prokopidis, Chambers and Ni Lochlainn41) . However, further longitudinal studies examining the effect of protein and fibre on appetite and energy intake in older adults are needed.

There is debate surrounding optimal protein sources to support healthy ageing. Although plant proteins are generally characterised by a lower content of essential amino acids, a meta-analysis of nine studies (including three studies in adults aged over 50 years) found longer-term supplementation with animal or plant protein combined with resistance exercise produced similar effects on lean mass and strength(Reference Messina, Lynch and Dickinson42). Furthermore, evidence from cell and animal models suggests that insoluble fibre may enhance de novo amino acid biosynthesis via alterations in the gut microbiome(Reference Prokopidis, Chambers and Ni Lochlainn41,Reference Martin, Ecklu-Mensah and Ha43) , which would support combining plant protein with fibre supplementation. Plant proteins are also well accepted by older adults and more environmentally sustainable(Reference Grasso, Hung and Olthof44,Reference Pimentel and Pimentel45) .

Consensus guidelines on nutrition for older adults highlight the importance of individualised nutrition interventions and recommend including additional non-dietary factors such as physical activity (PA) or social aspects(Reference Volkert, Beck and Cederholm2). In healthy older adults, most benefits of protein supplementation are only observed when combined with exercise(Reference Kirwan, Mazidi and Rodríguez García46). There is initial evidence that whey protein supplementation combined with exercise can increase energy intake in older adults(Reference Johnson, Holliday and Mistry36). Elsewhere, it has been hypothesised that increasing PA may benefit appetite and energy intake, although the evidence base to support this is currently limited(Reference Clegg and Godfrey47,Reference Crabtree, Cox and Lim48) .

The innovative plAnt Protein fibre and Physical activity solutions to address poor appEtite and prevenT undernutrITion in oldEr adults (APPETITE) randomised controlled trial (RCT) aims to determine the impact of a personalised optimised diet (including innovative plant protein fibre (PPF) products), a PA programme, and their combination on appetite and other nutritional, functional, metabolic and clinical outcomes in community-dwelling older adults. The multi-country trial is part of the European APPETITE project, funded under the Horizon Joint Programming Initiative ‘A Healthy Diet for a Healthy Life’(Reference Volkert, Corish and Dardevet49).

Methods and analysis

The protocol is written in accordance with the Standard Protocol Items: Recommendations for Interventional Trials (SPIRIT) guidelines(Reference Chan, Tetzlaff and Gotzsche50). A summary checklist is reported in Appendix 1(online Supplemental Appendix 1). The composition, roles and responsibilities of the coordinating centre, individuals overseeing the trial and external advisory board are listed in Appendix 2 (online Supplemental Appendix 2).

Study design

The trial is a multi-centre RCT aiming to recruit 180 community-dwelling older adults (about 60 per centre) in Nuremberg – Germany, Dublin – Ireland and Padua – Italy, all urban settings. Employing a 2 × 2 factorial parallel-group design, outcome measures will be assessed pre and post a 12-week intervention. Participants will be randomly allocated (1:1:1:1) by study centre and sex to one of four groups:

  1. (1) Personalised diet (PD): daily consumption of two PPF products and dietary counselling over a 12-week period;

  2. (2) PA: group exercise classes twice per week and home-based walking over a 12-week period;

  3. (3) PD and PA: both interventions described above combined;

  4. (4) Control: no intervention, usual diet and PA.

An overview of the timeline for participants is shown in Fig. 1.

Fig. 1. Overview of timing of screening, intervention and assessments. Primary outcomes are assessed at baseline and week 13. Created in Biorender.com

Screening (telephone followed by in-person) and baseline (pre-intervention) assessments will be completed within 6 weeks prior to commencing the trial. The intervention duration lasts 12 weeks. Post-intervention testing will be performed in the week following the intervention. In groups involving PD, participants will be required to consume PPF supplements and in groups involving PA to complete home-based walking up to and including the day prior to returning for the final outcome assessment, respectively.

Sample size

Sample size calculations were conducted in G * Power (version 3.1). A 120 kcal (500 kJ) difference in ad libitum test meal energy intake and a 10 mm change in visual analogue scale (VAS) appetite ratings have previously been considered physiologically relevant differences(Reference Blundell, De Graaf and Hulshof8,Reference Gregersen, Flint and Bitz51) . To allow for 20–25 % dropout, a sample size of 180 participants (45 per group) is sufficient to detect these differences between groups, allowing for 10 % variance on a within participant sd of change in ad libitum test meal energy intake of 143 kcal (Reference Johnson, Holliday and Mistry36,Reference Wijnhoven, Van Der Meij and Visser52) , and for VAS of about 13 mm, observed in our unpublished data, similar to others(Reference Johnson, Holliday and Mistry36), at 80 % power and significance at P < 0·05.

Recruitment and eligibility of study participants

Multiple recruitment strategies will be employed including flyers, social media and newspaper advertisements. If recruitment does not meet targets in one centre, this may be compensated for by additional recruitment at another centre. Interested individuals will be provided with a participant information sheet, and if still interested and potentially eligible will complete telephone screening with a trained researcher. Persons who are still eligible after telephone screening will subsequently be invited to complete an in-person screening at the study centre. Criteria to determine participant eligibility are shown in Table 1. Medical conditions and medications for exclusion are listed in Appendix 3 (online Supplemental Appendix 3). Due to initially very slow recruitment, age was lowered from originally >/= 70 years, a Simplified Nutritional Appetite Questionnaire (SNAQ) score </=14 removed (both April 2023) and BMI widened from 22 to 27 kg/m2 (August 2023). Most previous studies examining appetite in older groups and showing reduced appetite and energy intake compared with younger groups involved older adults aged 60–65 years and older(Reference Giezenaar, Chapman and Luscombe-Marsh10).

Table 1. APPETITE trial inclusion and exclusion criteria

MMSE, Mini Mental State Examination; CES-D, Centre of Epidemiology Study – Depression (CES-D) questionnaire; PA, physical activity.

Randomisation, blinding and study allocation

Participants will be randomised upon meeting all eligibility criteria on completion of in-person screening and will be informed of their allocated group after baseline data have been collected. Randomisation will be stratified by study centre and sex. If a participant is identified as ineligible after randomisation and prior to baseline assessment due to error in screening(Reference Fergusson53), a participant of the same sex will be randomised to the group the ineligible participant was allocated to. If members of the same household are eligible, they will be stratified to the same group. Randomisation will be centralised and conducted by an independent researcher, not connected to the project, using the QMINIM platform (Telethon Kids Institute, Australia). For the duration of the intervention and post-intervention assessments, both participants and researchers are unblinded to intervention allocation.

Interventions

Personalised diet

The PD intervention involves individual dietary counselling by a dietitian/trained nutritionist/research scientist and daily consumption of PPF products (detailed description below). The intervention aims at achieving the following predefined nutritional targets:

  1. (1) Daily consumption of 2 × 25 g PPF powders added to food/drinks.

  2. (2) Daily energy intake of 25–30 kcal/kg body weight(Reference Bernabei, Landi and Calvani54).

  3. (3) Daily protein intake of 1–1.2 g/kg body weight from food and PPF(Reference Reinders, Visser and Jyväkorpi55).

These nutritional goals are based on previous research in older adults(Reference Bernabei, Landi and Calvani54,Reference Reinders, Visser and Jyväkorpi55) . As recommended by expert consensus statements(Reference Volkert, Beck and Cederholm2), participants will be regularly monitored and nutritional targets will be adjusted according to each participant’s current nutritional status and co-morbidities requiring specific dietary strategies. One personalised dietary advice session (about 45 min) will be delivered in person at the start of the intervention, and two 35–45-min sessions via telephone (weeks 4 and 8). In addition, fortnightly compliance telephone calls will be conducted by a trained member of the research team. The personalised dietary advice will be based on the following assessments: (i) 3-d food diary (week before starting intervention, see below), (ii) nutritional assessment at baseline and (iii) two single 24-h dietary recalls via telephone (weeks 4 and 8).

As part of the nutritional counselling, participants will be provided with a ‘Hints and Tips’ booklet with suggestions, including recipes, on how to incorporate the PPF powders into their everyday foods/meals/snacks/beverages, preferably in meals, snacks and/or beverages that contain 6–7 g protein from other sources (e.g. 20–25 g meat, 40 g fish, one egg, glass of milk, 125 ml yogurt, 25 g cheese, 2 thick slices bread, 25 g almonds or Brazil nuts), to enhance circulating methionine, as methionine appearance was found to be limited following PPF consumption(Reference De Marco Castro, Valli and Buffière56). As a priority, participants will be instructed to include a full 25 g sachet of PPF powder at two meals where protein intake is identified as being low (e.g. breakfast and lunch), to optimise protein distribution(Reference Murphy, Oikawa and Phillips20). Participants will only be advised to spread the two sachets across multiple eating occasions if they report significant difficulty with consuming a full PPF sachet at one meal.

Where needed, participants will also be provided with country-specific resources that provide simple advice on how to address poor appetite and meet energy requirements to support the participant achieving a daily dietary intake of 25–30 kcal/kg and 1–1·2 g protein/kg body weight., for example, Nutrition supports – HSE.ie(57).

Description of plant protein fibre products

Initially six varieties of PPF blends from different plant sources were developed by Fraunhofer Institute for Process Engineering and Packaging (IVV) (Freising, Germany) as part of the APPETITE project(Reference Volkert, Corish and Dardevet49). The PPF blends were designed to provide equivalent leucine and closely matched branched chain and indispensable amino acids and align with optimal values described for older adults to promote muscle mass and strength(58). Their acceptability in a food matrix (natural yogurt) and sensory properties were subsequently tested by older adults (> 65 years, n 25) at two trial centres (FAU, Germany and UCD, Ireland). The three blends with the greatest acceptability had mean (sd) Likert scale (0–9 point) scores of 5 (2), corresponding to ‘neither like nor dislike’, similar to acceptability of oral nutritional supplements in older adults reported in previous studies(Reference Regan, O’Neill and Hutchings59).

These three PPF blends were subsequently investigated for circulating plasma amino acid appearance following ingestion of the products in older adults, with results reported elsewhere, including quantitatively measured amino acid composition of the blends(Reference De Marco Castro, Valli and Buffière56). Based on these findings, two blends (referred to as PPF A and PPF B) were selected for the RCT. PPF A consists of 54 % pea protein isolate, 17 % oat protein concentrate, 9 % almond protein concentrate and 20 % vegetable pea fibre, with a 25 g sachet providing 15·3 g protein and 3·6 g fibre. PPF B consists of 36 % pea protein isolate, 26 % soya protein isolate, 18 % rice protein isolate and 20 % vegetable pea fibre, with a 25 g sachet providing 17·1 g protein and 3·6 g fibre. The ingredients used for the PPF formulation are commercial protein ingredients resulting from dry and wet fractionation of plant raw materials. The fibre ingredient is a commercial product derived from pea kernels after protein extraction. The protein contents of the ingredients and the nutritional composition of the PPF are provided in more detail in the previous publication of de Marco Castro et al. (Reference De Marco Castro, Valli and Buffière56) and in Appendix 4. Participants will be given the same quantity of each PPF and advised to consume one sachet of each type per d.

Physical activity

The PA intervention involves group exercise classes in a supervised setting twice per week (with at least 48 h between training sessions) and home-based walking three times per week, following a similar format to previous multi-centre trials in community-dwelling older adults (Reference Bernabei, Landi and Calvani54,Reference Pahor, Guralnik and Ambrosius60) .

The group exercise class will begin with a warm-up including training on walking dynamics. This will be followed by approximately 3–4 balance exercises. Resistance exercise will then be conducted in line with guidelines for resistance exercise in older adults(Reference Hurst, Robinson and Witham61). Upper and lower body exercises will be completed using adjustable weights across centres including the following exercises: wide leg squat, standing leg curl, hip flexion, knee extension, seated row, bicep curls, seated shoulder press, along with push-ups (against a wall). The exercise intensity will progressively increase so that all participants should be achieving an intensity of 15 to 16 on the Borg 6–20 rate of perceived exertion (RPE) scale(Reference Borg62). Weights will be increased individually so that this intensity is maintained throughout the remainder of the programme. For each strength exercise, participants will be instructed to perform 8–12 repetitions (one set), rest for approximately 1 min and then perform subsequent sets. The sets and repetitions prescribed will progressively increase over the 12-week programme. For example, in week 1, participants will perform eight repetitions (one set) per exercise, rest for approximately 1 min and then perform a second set. As the participants progress, repetitions will increase from 8 to 10 to 12 and sets will increase from 2 to 3 sets per exercise.

For home-based walking, the goal is 60 min (3 × 20 min) of walking per week during the first 3 weeks, 90 min (3 × 30 min) per week for weeks 4–6 and finally 120 min (3 × 40 min) per week for weeks 7–12. The walking goals may be accumulated over the day until participants are able to achieve the continuous duration. Walking pace should be at a moderate intensity defined as an RPE of 13 on the Borg 6–20 scale(Reference Borg62). For individuals who are very deconditioned, it is acceptable to exercise at an RPE < 11 in the initial 3 weeks until they become more comfortable with the exercise protocol.

Personalised diet and physical activity

Participants in the personalised diet and physical activity (PD + PA) group will undertake both PD and PA interventions combined. Participants will follow identical procedures to those described in the PD and PA interventions above.

Control

The control group will receive no intervention, and participants are instructed to maintain their usual diet and PA which is considered standard care for older adults with poor appetite across study centres. Participants will be provided with tailored nutritional and lifestyle information following study completion.

Maximising and monitoring compliance with personalised diet and physical activity interventions

Adequate weekly compliance in the PD group is defined as self-reported consumption of at least ten of a possible fourteen PPF powder sachets in that week, similar to previous supplementation studies(Reference Bauer, Verlaan and Bautmans63). Participants will be asked to complete a daily log, ticking a box to indicate that they have consumed each powder sachet. In addition, participants will be asked to keep all empty sachets in a container provided by the research team at the baseline test visit, as an additional objective measure of compliance. This must be returned at the end of the study. Overall compliance is defined as adequate compliance for at least 9 weeks during the 12-week intervention (75 %).

During the fortnightly compliance telephone calls in the PD and PD + PA groups, compliance with the intervention will be encouraged and problems troubleshooted. For participants in the PD + PA group, this may instead be conducted in person before/after an exercise class, and for participants in the PA group it will be conducted in person before/after an exercise class to reduce participant burden.

Adequate compliance in PA groups is defined as completing a minimum of 75 % of group exercise sessions (i.e. a minimum of eighteen out of twenty-four sessions). Attendances will be recorded by the instructor at all supervised sessions. Home-based walking and all moderate to vigorous activity will be recorded in the compliance log. Compliance logs will be checked by trained researchers throughout the intervention at exercise sessions.

If participants do not adhere to the above interventions, they will be included in intention-to-treat analysis and excluded from per-protocol analysis.

Data collection and study outcomes

Data will be collected on two separate test visits at baseline and two identical visits post-intervention (week 13) (Fig. 1). One visit consists primarily of assessment of physical characteristics and function, and the other visit consists of an appetite test meal challenge. Participants will be instructed to avoid strenuous exercise and alcohol in the 24 h before testing on both occasions. Participants will also be instructed to fast for at least 10 h overnight, prior to arrival at the laboratory, and to consume nothing other than water during this time. A small glass of water is advised upon waking on the morning of testing. Participants will be instructed to follow their normal medication routine, and any smokers that are eligible will be instructed to avoid smoking/vaping on the morning of testing. A standardised snack will be provided to participants prior to physical function testing. For post-intervention testing, identical procedures will be followed. A summary of the data collection variables/measures and time points of collection is shown in online Supplemental Appendix 5.

Primary outcomes

Subjective appetite and ad libitum test meal energy intake

The joint primary outcomes are (i) postprandial composite appetite score (area under the curve from 0 to 180 min (AUC0–180 min)) derived from three 100 mm VAS (hunger, fullness and desire to eat) and (ii) energy intake (kilocalories (kcal)) from an ad libitum lunch test meal. Appetite ratings will be assessed at the following time points: fasting before (t –10 min) and after a standardised breakfast (see below) (0 min, 30 min, 60 min, 120 min, 180 min and post-lunch). This time frame represents a typical inter-meal interval during which time an oscillating pattern of hunger and fullness would be expected(Reference Gibbons, Finlayson and Dalton64,Reference Turicchi, O’Driscoll and Finlayson65) . Composite appetite score is calculated as follows: (VAS hunger + VAS fullness (100-rating) + VAS desire to eat)/3. On either end of the VAS 100 mm line are opposing terms (i.e. ‘not at all’ and ‘extremely’). The trapezoid method will be used for the calculation of AUC. The ad libitum test meal will be served at 180 min and energy intake will be assessed.

The joint primary outcomes were selected to include a subjective and an objective measure of appetite, reflecting different processes of appetite control(Reference Gibbons, Finlayson and Dalton64). VAS have a history of widespread use and acceptance across many countries and laboratories, and according to consensus recommendations, they are easily used and translated and appear to be a valid, sensitive and unbiased measurement tool of appetite(Reference Blundell, De Graaf and Hulshof8). VAS have been validated for assessment of appetite, including in older adults(Reference Flint, Raben and Blundell66Reference Parker, Ludher and Khai Loon68).

Test meals

The fixed breakfast meal consists of white bread toasted (88 kcal), butter (36 kcal), jam (24 kcal), orange juice (82 kcal) and strawberry yogurt (111 kcal), providing approximately 340 kcal overall, 57 g carbohydrate (66 % energy), 8 g fat (22 % energy) and 11 g protein (12 % energy) across all centres.

The ad libitum lunch test meal consists of a homogenous pasta-bake meal, identified as being acceptable to older adults across all centres. The key ingredients are pasta, tomato-based pasta sauce, cheese and olive oil, providing approximately 1900 kcal, 17 % energy protein, 54 % energy carbohydrate, 28 % energy fat (maximum 1 % energy deviation between centres). The meal is freshly prepared and provided in a large serving dish with utensils and a bowl into which participants help themselves. Participants are instructed that they have 30 min to help themselves to and eat as much as they wish until they feel comfortably full. Water intake is recorded and the amount of food consumed is determined by weighing the meal before and after consumption. Energy intake is calculated using the manufacturers’ energy values.

Secondary outcomes

Anthropometric measurements and body composition

Height, weight and seated maximum calf circumference of the dominant leg will be measured in duplicate using a stadiometer, digital scale and flexible measuring tape, respectively. Body resistance at 50 kHz will be measured by bioelectrical impedance analysis (BIA) at all sites as follows: Germany: (Impedimed Imp SFB7, Impedimed Limited, Queensland, Australia), Ireland: Bodystat QuadScan 4000, Bodystat Ltd, UK; Italy: BIA 101 BIVA® PRO, Akern Systems, Firenze, Italy) in a fasted state. Appendicular skeletal muscle mass, fat mass and fat-free mass will be estimated using validated equations in older adults(Reference Kyle, Genton and Karsegard69,Reference Sergi, De Rui and Veronese70) . Fat mass and fat-free mass will additionally be assessed by air displacement plethysmography (BodPod, Cosmed, Italy) at one site (Ireland), and fat mass, fat-free mass and appendicular skeletal muscle mass by dual-energy X-ray absorptiometry at one site (Italy).

Simplified Nutritional Appetite Questionnaire

Appetite will also be assessed via SNAQ(Reference Wilson, Thomas and Rubenstein71), a self-administered questionnaire adapted from the Appetite, Hunger and Sensory Perception questionnaire(Reference Mathey72). The four-item SNAQ includes questions on appetite, fullness, taste and frequency of eating and has been shown to predict weight loss in community-dwelling older adults(57). It will be completed at baseline during in-person screening and post-intervention on the test day assessing physical characteristics and function.

Fasting appetite ratings

Fasting appetite ratings for hunger, fullness and desire to eat will be assessed using 100 mm VAS prior to consumption of the fixed breakfast meal.

Palatability of test meals

Palatability of the breakfast and lunch meals will be assessed using six 100 mm VAS. Questions include how pleasant was the meal, how satisfying was the meal, how tasty was the meal, how filling was the meal, how sweet was the meal and how savoury was the meal. Each end of the VAS is anchored with the words ‘not at all’ and ‘extremely’.

Dietary intake

Energy, protein and fibre intake will be assessed using a 3-d non-weighed food diary administered at baseline (pre-intervention) and in the final week of the intervention or control period. Participants will be instructed orally and in written form to record all items of food and beverages consumed and provide details of the brand, estimated quantity and cooking methods used. Energy and nutrient intake will be calculated using national nutrient databases (73,Reference Gnagnarella, Salvini and Parpinel74) .

Cardiorespiratory fitness, physical function and strength

Cardiorespiratory fitness will be estimated using a usual-paced 400 m walk test(Reference Moffit, Qiao and Moored75). Physical function will be assessed by Short Physical Performance Battery (SPPB) combining the assessment of balance, gait speed and repeated chair stands tests(Reference Guralnik, Simonsick and Ferrucci76). Individual test scores and overall score will be calculated. Leg strength of the dominant leg will be assessed as the maximum value from three trials using a seated leg extension dynamometer to determine maximal voluntary isometric contraction of the knee extensors. Handgrip strength will be assessed as the maximum value from three trials with a Jamar hydraulic grip strength dynamometer, with the participant in a seated position and arm rested on the table at a 90-degree angle using the dominant hand, unless contraindicated.

Physical activity

PA and sedentary behaviour (including steps and METs, time spent walking, sedentary time and sit to stand transitions per d) will be assessed by ActivPAL accelerometer (activPAL3TM micro, or activPAL4; PAL Technologies Ltd). The participant will be provided with the accelerometer to wear on the midline of the thigh for 7 d at baseline prior to commencing the intervention and during week 12 of the intervention or control period. Participants will also complete the Physical Activity Scale for the Elderly (PASE) questionnaire(Reference Washburn, Smith and Jette77). The PASE questionnaire is a brief and easily scored survey designed specifically to assess PA duration, frequency and exertion over a 7-d period in individuals 65 years and older. At post-intervention, participants will be instructed to include activities undertaken as part of the intervention in their response.

Resting energy expenditure

Resting energy expenditure (kcal/d) will be assessed following an overnight fast in participants at one site (Ireland) using indirect calorimetry (Q-NRG, Cosmed).

Cognitive status, dietary restraint and depressive symptoms

Cognitive status will be assessed by Mini Mental State Examination (MMSE)(Reference Folstein, Folstein and McHugh78). Cognitive dietary restraint will be assessed using the cognitive dietary restraint subscale of the Three-Factor Eating Questionnaire (TFEQ)(Reference Stunkard and Messick79). The subscale consists of six ‘true/false’ and Likert scale-type questions relating to cognitive dietary restraint from the original fifty-item questionnaire. Depressive symptoms will be assessed by Centre of Epidemiology Study – Depression (CES-D) questionnaire(Reference Radloff80).

Quality of life

Subjective rating of perceived Quality of Life will be assessed using the EuroQol (European Quality Of Life) questionnaire (EQ-5D-5L)(Reference Herdman, Gudex and Lloyd81). This consists of self-assessed rating of health under five dimensions (Mobility, Self-Care, Usual Activity, Pain/Discomfort, Anxiety/Depression) and perceived overall health on a VAS (0–100) anchored with opposing statements (0= the worst health you can imagine; 100= the best health you can imagine).

Blood biochemical measures

A fasting venous blood sample will be collected from participants at all sites prior to consumption of the fixed breakfast meal at baseline and post-intervention. Serum, lithium heparin and EDTA aprotinin tubes will be collected, processed according to standardised protocols and samples stored in aliquots at –80°C until analysis. Biomarkers related to appetite including ghrelin, GLP-1, PYY, glucose, insulin and leptin will be analysed centrally at one site (Ireland), except for plasma samples which will be transferred to National Research Institute for Agriculture, Food and the Environment (INRAE), France, for metabolomic analysis.

Postprandial samples in response to the fixed breakfast meal will also be collected at one site (Ireland) at baseline and post-intervention. Along with fasting measures, appetite-related gut hormones (ghrelin, glucagon-like peptide-1 (GLP-1) and peptide YY (PYY) will be assessed at 30, 60, 120 and 180 min post-breakfast until the ad libitum lunch test meal is served at 180 min and analysed in Ireland. In addition, metabolomic analysis will be conducted at INRAE, France, on postprandial samples collected at the same time points. At each site, all samples will be analysed together upon completion of the trial.

Gut microbiome diversity and gut metabolomic profiles

Gut microbiome diversity and metabolomic profiles will be assessed from a faecal sample and faecal water collected at baseline and post-intervention from participants at two sites (Ireland and Germany). Samples will be stored at –80°C until being analysed centrally (Ireland) after completion of the trial. Gut microbiome diversity will be assessed using 16S rRNA sequencing.

Muscle motor unit behaviour and muscle signalling

Motor unit behaviour(Reference Valli, Sarto and Casolo82) will be determined by high-density electromyography on the vastus lateralis muscle (OT Bioelettronica) at one site (Italy). The primary outcome variables extracted from high-density electromyography will be motor unit mean discharge rate (pps), including discharge rate at recruitment/plateau/de-recruitment, muscle fibre conduction velocity (m/s) and persistent inward currents.

Muscle signalling related to muscle plasticity, metabolism, denervation and capillarisation will also be determined from muscle biopsies, at baseline and post-intervention, from participants who consent at one site (Italy). Biopsies will be taken using MEDAX/BF14100-C0; Bio-Feather with coaxial 14 g 10 cm and subsequently stored at −80°C. Sample analysis will be performed after completion of the trial. The following parameters will then be measured in the sample using western blot with specific antibodies for total proteins or by their activated phosphorylated form: (1) markers of denervation (AChR; agrin/MuSK/Lrp4, NCAM, Myog); (2) markers of protein turnover (atrogin1, MURF1, LC3, BNIP3, Akt-dependent mTOR and FoxO); (3) markers of mitochondrial dynamics (OPA1, DRP1); and (4) markers of energy metabolism pathways (AMPK and PGC1alpha).

Acceptability of the trial

To determine acceptability and feasibility of the intervention and overall experience while enrolled in the study, a study-specific questionnaire designed similar to previous studies(Reference Niskanen, Reinders and Wijnhoven83) containing statements (e.g. I was able to integrate the programme into everyday life) and five-point Likert scale responses ranging from ‘Strongly disagree’ to ‘Strongly agree’ will be administered to participants on completion of the intervention. The questionnaire will also enable participant challenges and suggestions to be reported through open questions (e.g. What helped you (or made it difficult) to follow through with the programme?). In addition, for participants in the PD groups, feedback on the PPF products will be recorded at the end of the intervention and during the dietary recall telephone calls with open questions (e.g. How did you integrate the PPF products into your diet?).

Adverse effects and events

Any adverse effects will be recorded as reported by participants during the trial, for example, during fortnightly telephone calls for PD groups, during PA classes or if a participant contacts the research team to report adverse effects or events at any time during the trial.

Data management and statistical analysis plan

All data will be collected on questionnaires and record sheets in a de-identified manner using a participant ID number and stored securely according to General Data Protection Regulation (2018)(84) at each site, with electronic data double-entry into a central electronic database stored and backed up at one site (Ireland). The trial coordinating centre Principal Investigators will have access to the full dataset across all sites. Study site Principal Investigators will have direct access to the dataset at their own site and will have access to data from other sites by request. Anonymised data will be made available to other researchers on reasonable request after the main trial manuscript is published.

There are no plans for interim study analysis. After completion of the study data collection, data will be checked and cleaned using descriptive statistics and data visualisation. Outcome data will first be analysed according to the intention-to-treat principle, using a random coefficients generalised linear mixed model for primary and secondary end points. The effects of time, the two interventions and their interaction (following the 2 × 2 factorial design of the trial) and sex will be included as fixed effects. Participant ID and study site will be included as random effects. Residuals will be tested for normality and transformation applied where required, or where the structure of the data is inherently non-normal. 95 % CI will be reported where applicable. Per-protocol analyses and mediation analyses will be conducted to examine to what extent compliance and potential mediating mechanisms explain the impact on the primary and secondary end points. For primary pre-planned contrasts, significance will be accepted as P < 0·05. Where groups of secondary outcomes are analysed, the significance level will be adjusted by Bonferroni correction according to the number of responses in the analysis. A correlation matrix will be constructed to assess relationships between outcome variables. Missing data will not be imputed in the primary analysis. Intention-to-treat analyses will be based on the as-observed population.

Ethics and dissemination

Ethical approval has been received from the Human Research Ethics Committees at each trial centre and the trial registered on ClinicalTrials.gov (NCT05608707). The study will be reported according to the Consolidated Standards of Reporting Trials (CONSORT) guidelines for parallel-group randomised trials. Participant informed consent will be obtained in writing prior to study enrolment (online Supplemental Appendix 6). Adverse events will be recorded and reported to the relevant ethics committee. Participants are informed they may withdraw with no obligation to provide a reason. If participants choose to provide a reason, the reason will be recorded. Amendments to the trial protocol including changes to study objectives, design, participant population, sample sizes, study procedures or significant administrative aspects are updated on the trial registry and submitted as an amendment for ethical approval at each site.

Trial results will be disseminated through websites, reports, presentations, peer-reviewed journal articles and workshops to a wide audience of stakeholders in the area of healthy ageing including researchers, healthcare providers, policymakers, industry and older adults. Topics and authors proposed for peer-reviewed publication as a journal article will be circulated to the trial principal investigators of the coordinating centres and the consortium principal investigators, with authorship based on established authorship guidelines(85).

Discussion

The APPETITE trial is the first RCT to evaluate the impact of PD and PA alone or in combination on appetite and related health outcomes in older adults. The PD intervention involves the participant incorporating two PPF powder supplements into the diet and receiving personalised dietary advice to achieve defined daily energy and protein targets. The PA intervention involves supervised resistance exercise classes twice per week and home-based walking three times per week.

Although previous studies have investigated the effects of protein supplementation, alone or with PA on sarcopenia-related outcomes(Reference Hou, Lei and Li86,Reference ten Haaf, Nuijten and Maessen87) , nutritional outcomes, particularly appetite, have received little attention. Alongside plant protein supplementation, the inclusion of fibre, identified as lacking in diets of many older adults and appealing to those with poor appetite(Reference Kehoe, Walton and Flynn26,Reference Van Der Meij, Wijnhoven and Lee27,Reference Van Der Meij, Wijnhoven and Finlayson35,Reference Ter Borg, Verlaan and Mijnarends88) , is a novel aspect of the present study. Furthermore, previous supplementation studies have focused primarily on providing a supplement, without considering usual dietary habits and preferences, thus not following a personalised approach which is recommended by consensus guidelines(Reference Volkert, Beck and Cederholm2).

The PPF supplements that are provided to participants as part of the PD intervention were developed based on prior research and initial data from earlier work packages as part of the wider APPETITE project(Reference Volkert, Corish and Dardevet49). The supplements provided consist of a blend of plant proteins to optimise the amino acid content and reduce the limitations associated with providing a single plant protein source(Reference Pinckaers, Trommelen and Snijders89). The PPF supplements were selected from a range of six blends developed for the trial, initially based on results from sensory testing among older adults to optimise compliance, and subsequently from assessment of peripheral amino acid appearance following consumption.

As noted in the methods section, during the initial months of the trial, the inclusion criteria requiring participants to have a SNAQ score </= 14 was removed. This criterion was adjusted for several reasons including difficulty encountered in recruitment and acknowledging both findings from work package 1 of the wider APPETITE project and limited validation studies of SNAQ as an assessment of appetite per se. Work package 1 involved semi-structured interviews with older adults with ‘poor appetite’ as defined by SNAQ (</=14). A key finding was that despite their SNAQ score, many participants did not recognise they had a poor appetite or were reluctant to acknowledge their appetite loss(Reference Dismore, Sayer and Robinson90). This difficulty in self-identifying appetite loss may likely contribute to challenges in recruiting community-dwelling older adults with a ‘poor appetite’. While the inclusion of specific ‘appetite loss’ criteria may be more feasible in a clinical setting (where appetite loss is more widespread and more pronounced) as part of regular patient screening and appropriate for drug trials, such criteria may be less applicable for lifestyle intervention trials targeting community-dwelling older adults. In addition, reduced appetite and energy intake occurs in healthy older compared with younger adults(Reference Giezenaar, Chapman and Luscombe-Marsh10), and is not defined by SNAQ score specifically. Consequently, the APPETITE trial will include older adults not defined by a specific ‘appetite status’ at baseline.

A key strength of the design is the multi-centre design, thereby enhancing the generalisability of findings and potential future implementation of the interventions. Further strengths include the 2 × 2 design, allowing for the impact of PD and PA separately and in combination to be elucidated. In addition, given additional facilities and expertise available at some centres (such as muscle biopsy and analysis), insight into important additional outcomes will be obtained in subsamples. The integration of comprehensive assessment, including body composition, gut microbiome, blood biomarkers, functional, metabolic and health-related outcomes, will give insight into mechanisms contributing to any changes observed.

The time required to improve some of the outcomes assessed is unclear and may require a longer duration than the 12-week intervention in the APPETITE RCT; however, effects of protein supplementation and exercise on appetite have previously been demonstrated in 12-week trials across various populations(Reference Johnson, Holliday and Mistry36,Reference King, Caudwell and Hopkins91) .

Due to the nature of the intervention, one limitation is that it is not possible to blind participants to treatment allocation. An additional limitation is the lack of blinding of researchers who are involved in both the administration of the intervention and data collection due to logistical constraints. However, data will be analysed anonymously by a blinded researcher to minimise detection bias.

In summary, the APPETITE multi-centre RCT will provide novel insight on the impact of PD (incorporating PPF products), PA and their combination on appetite, and other nutritional, functional, clinical and metabolic outcomes in community-dwelling older adults. This will advance knowledge on how these interventions influence appetite, dietary intake and nutritional status and contribute to future research in the field. This will ultimately inform guidelines to contribute to a better nutritional status and quality of life for older Europeans.

Trial status

This protocol is version 4 registered on 29/9/2023. Recruitment began in September 2022 and finished in April 2024, with the last participant completing their final test visit in July 2024.

Acknowledgements

The authors would like to thank the study participants, those who have assisted with recruitment and Professsor Ellen Freiberger for guidance regarding conducting the PA programme.

This study is part of the European Joint Programming Initiative ‘A Healthy Diet for a Healthy Life’ (JPI HDHL) and the ERA-NET Cofund ERA-HDHL (GA N° 696295 of the EU Horizon 2020 Research and Innovation Programme) project APPETITE. The funding agencies supporting this RCT in the APPETITE project are (in alphabetical order of participating Member State) France: French National Research Agency (ANR) (), Germany: Federal Ministry of Food and Agriculture (BMEL) represented by Federal Office for Agriculture and Food (BLE) (), Ireland: The Health Research Board (HRB), email: and Italy: Ministero dell’Università e della Ricerca (MUR) (). The funders have no involvement in study design, collection of data, management, analysis and interpretation of data or decision to submit for publication.

Conceptualisation: C. C., K. H., G. D. V., D. V. and M. V.; Data curation: M. B., F. G., K. H., B. M., A. Q., P. S. and W. S.; Funding acquisition: C. C., D. D., C. G., K. H., G. D. V., D. V. and M. V.; Investigation: M. B., F. G., B. M., A. Q., P. S. and W. S.; Methodology: C. C., S. G., K. H., B. M., J. P., A. Q., W. S., P. S., D. V. and M. V.; Project administration: B. M., C. C., K. H., A. Q., G. D. V., D. V. and M. V.; Supervision: C. C., K. H., G. D. V., D. V. and M. V.; writing – original draft: K. H.; and writing – review and editing: all authors. All authors approved the final article.

The principal investigators for the overall trial and each study site have no conflicts of interest to declare.

Ethical approval has been received at all trial sites: Ireland: University College Dublin Human Research Ethics Committee (LS-21-96-Roche); Germany: Ethics committee of the Medical Faculty of the FAU (22-67-S); Italy: Ethics Committee for Experimentation with Human Beings of the Department of Biomedical Science, University of Padua (HEC-DSB/02-22).

Anonymised data will be made available to other researchers on reasonable request after the end of the study.

Supplementary material

For supplementary material/s referred to in this article, please visit https://doi.org/10.1017/S0007114524002125

Footnotes

These authors contributed equally to this work.

Trial registration number Clinical Trials.gov Registry NCT05608707

Date: 09/08/23

Version Identifier: 04, Changes to inclusion criteria April 2023, August 2023, noted page 9

Funding: Funded under the Horizon Joint Programming Initiative ‘A Healthy Diet for a Healthy Life’

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Figure 0

Fig. 1. Overview of timing of screening, intervention and assessments. Primary outcomes are assessed at baseline and week 13. Created in Biorender.com

Figure 1

Table 1. APPETITE trial inclusion and exclusion criteria

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