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7. Anticancer actions of carnosine in cellular models of prostate cancer.

Author

Habra, K., Pearson, J. R. D., Le Vu, P., Puig‐Saenz, C., Cripps, M. J., Khan, M. A., Turner, M. D., Sale, C., and McArdle, S. E. B.

Subjects
HIGH-intensity focused ultrasound, PROSTATE cancer, EXTERNAL beam radiotherapy, CARNOSINE, RADICAL prostatectomy
Abstract

Treatments for organ‐confined prostate cancer include external beam radiation therapy, radical prostatectomy, radiotherapy/brachytherapy, cryoablation and high‐intensity focused ultrasound. None of these are cancer‐specific and are commonly accompanied by side effects, including urinary incontinence and erectile dysfunction. Moreover, subsequent surgical treatments following biochemical recurrence after these interventions are either limited or affected by the scarring present in the surrounding tissue. Carnosine (β‐alanyl‐L‐histidine) is a histidine‐containing naturally occurring dipeptide which has been shown to have an anti‐tumorigenic role without any detrimental effect on healthy cells; however, its effect on prostate cancer cells has never been investigated. In this study, we investigated the effect of carnosine on cell proliferation and metabolism in both a primary cultured androgen‐resistant human prostate cancer cell line, PC346Flu1 and murine TRAMP‐C1 cells. Our results show that carnosine has a significant dose‐dependent inhibitory effect in vitro on the proliferation of both human (PC346Flu1) and murine (TRAMP‐C1) prostate cancer cells, which was confirmed in 3D‐models of the same cells. Carnosine was also shown to decrease adenosine triphosphate content and reactive species which might have been caused in part by the increase in SIRT3 also shown after carnosine treatment. These encouraging results support the need for further human in vivo work to determine the potential use of carnosine, either alone or, most likely, as an adjunct therapy to surgical or other conventional treatments. [ABSTRACT FROM AUTHOR]

Published
2024
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9. Modelling Changes in Bone and Body Composition Over a Season in Elite Male Footballers

Author

Varley, I, Ward, M, Thorpe, C, Beardsley, N, Greeves, J, Sale, C, and Saward, C

Subjects
Male, Absorptiometry, Photon, Bone Density, Body Composition, Football, Humans, Orthopedics and Sports Medicine, Physical Therapy, Sports Therapy and Rehabilitation, Seasons
Abstract

This study investigated the change in bone and body composition characteristics of elite football players and recreationally active control participants across the course of a season. Fortysix participants (20 footballers and 26 recreationally active controls) were assessed by dual-energy x-ray absorptiometry and peripheral Quantitative Computed Tomography for a range of bone and body composition characteristics at four points over the course of a competitive season. Multilevel modelling was used to examine changes. Footballers had higher characteristics than controls for 24 out of 29 dual-energy x-ray absorptiometry and peripheral Quantitative Computed Tomography variables (all p

Published
2022

10. Correction to: Bone mineral density in high-level endurance runners: part A—site-specific characteristics

Author

Herbert, AJ, Williams, AG, Lockey, SJ, Erskine, RM, Sale, C, Hennis, PJ, Day, SH, Stebbings, GK, Herbert, AJ, Williams, AG, Lockey, SJ, Erskine, RM, Sale, C, Hennis, PJ, Day, SH, and Stebbings, GK

Abstract

The original version of this article unfortunately contained a mistake. Figure 1C was missing The corrected Fig. 1 should have appeared as shown in the following page. The original article has been corrected.

Published
2022

11. Bone mineral density in high-level endurance runners: Part B—genotype-dependent characteristics

Author

Herbert, AJ, Williams, AG, Lockey, SJ, Erskine, RM, Sale, C, Hennis, PJ, Day, SH, Stebbings, GK, Herbert, AJ, Williams, AG, Lockey, SJ, Erskine, RM, Sale, C, Hennis, PJ, Day, SH, and Stebbings, GK

Abstract

Purpose Inter-individual variability in bone mineral density (BMD) exists within and between endurance runners and non-athletes, probably in part due to differing genetic profiles. Certainty is lacking, however, regarding which genetic variants may contribute to BMD in endurance runners and if specific genotypes are sensitive to environmental factors, such as mechanical loading via training. Method Ten single-nucleotide polymorphisms (SNPs) were identified from previous genome-wide and/or candidate gene association studies that have a functional effect on bone physiology. The aims of this study were to investigate (1) associations between genotype at those 10 SNPs and bone phenotypes in high-level endurance runners, and (2) interactions between genotype and athlete status on bone phenotypes. Results Female runners with P2RX7 rs3751143 AA genotype had 4% higher total-body BMD and 5% higher leg BMD than AC+CC genotypes. Male runners with WNT16 rs3801387 AA genotype had 14% lower lumbar spine BMD than AA genotype non-athletes, whilst AG+GG genotype runners also had 5% higher leg BMD than AG+GG genotype non-athletes. Conclusion We report novel associations between P2RX7 rs3751143 genotype and BMD in female runners, whilst differences in BMD between male runners and non-athletes with the same WNT16 rs3801387 genotype existed, highlighting a potential genetic interaction with factors common in endurance runners, such as high levels of mechanical loading. These findings contribute to our knowledge of the genetic associations with BMD and improve our understanding of why some runners have lower BMD than others.

Published
2022

12. Beta-alanine did not improve high-intensity performance throughout simulated road cycling

Author

Perim, P, Gobbi, N, Duarte, B, Oliveira, LFD, Costa, LAR, Sale, C, Gualano, B, Dolan, E, Saunders, B, Perim, P, Gobbi, N, Duarte, B, Oliveira, LFD, Costa, LAR, Sale, C, Gualano, B, Dolan, E, and Saunders, B

Abstract

This study investigated the effect of beta-alanine supplementation on short-duration sprints and final 4-km simulated uphill cycling time-trial performance during a comprehensive and novel exercise protocol representative of the demands of road-race cycling, and determined if changes were related to increases in muscle carnosine content. Seventeen cyclists (age 38 ± 9 y, height 1.76 ± 0.07 m, body mass 71.4 ± 8.8 kg, V̇O2max 52.4 ± 8.3 ml·kg−1·min−1) participated in this placebo-controlled, double-blind study. Cyclists undertook a prolonged intermittent cycling protocol lasting 125 min, with a 10-s sprint every 20 min, finishing with a 4-km time-trial at 5% simulated incline. Participants completed two familiarization sessions, and two main sessions, one pre-supplementation and one post-supplementation following 28 days of 6.4 g·day−1 of beta-alanine (N=11) or placebo (N=6; maltodextrin). Muscle biopsies obtained pre- and post-supplementation were analysed for muscle carnosine content. There were no main effects on sprint performance throughout the intermittent cycling test (all P>0.05). There was no group (P=0.69), time (P=0.50) or group x time interaction (P=0.26) on time-to-complete the 4-km time-trial. Time-to-completion did not change from pre- to post-supplementation for BA (−19.2 ± 45.6 s, P=0.43) or PL (+2.8 ± 31.6 s, P=0.99). Beta-alanine supplementation increased muscle carnosine content from pre- to post-supplementation (+9.4 ± 4.0 mmol·kg−1dm; P<0.0001) but was not related to performance changes (r=0.320, P=0.37). Chronic beta-alanine supplementation increased muscle carnosine content but did not improve short-duration sprint performance throughout simulated road race cycling, nor 4-km uphill time-trial performance conducted at the end of this cycling test. Highlights Performance during prolonged cycling events often depends on the ability to maintain an increased power output during higher intensity periods. Thus, cyclists are likely heavily dependent o

Published
2022

19. Nutrition and Athlete Bone Health

Author

Sale, C and Elliott-Sale, KJ

Subjects
Gerontology, medicine.medical_specialty, Bone density, Sports medicine, Osteoporosis, Population, 030209 endocrinology & metabolism, Physical Therapy, Sports Therapy and Rehabilitation, Review Article, Bone and Bones, vitamin D deficiency, 03 medical and health sciences, 0302 clinical medicine, Bone Density, Dietary Carbohydrates, medicine, Humans, Orthopedics and Sports Medicine, Vitamin D, education, education.field_of_study, biology, Athletes, business.industry, Nutritional Requirements, 030229 sport sciences, Vitamin D Deficiency, medicine.disease, biology.organism_classification, Sports Nutritional Physiological Phenomena, Calcium, Dietary, Osteopenia, Dietary Proteins, Energy Intake, Energy Metabolism, business
Abstract

Athletes should pay more attention to their bone health, whether this relates to their longer-term bone health (e.g. risk of osteopenia and osteoporosis) or their shorter-term risk of bony injuries. Perhaps the easiest way to do this would be to modify their training loads, although this advice rarely seems popular with coaches and athletes for obvious reasons. As such, other possibilities to support the athletes’ bone health need to be explored. Given that bone is a nutritionally modified tissue and diet has a significant influence on bone health across the lifespan, diet and nutritional composition seem like obvious candidates for manipulation. The nutritional requirements to support the skeleton during growth and development and during ageing are unlikely to be notably different between athletes and the general population, although there are some considerations of specific relevance, including energy availability, low carbohydrate availability, protein intake, vitamin D intake and dermal calcium and sodium losses. Energy availability is important for optimising bone health in the athlete, although normative energy balance targets are highly unrealistic for many athletes. The level of energy availability beyond which there is no negative effect for the bone needs to be established. On the balance of the available evidence it would seem unlikely that higher animal protein intakes, in the amounts recommended to athletes, are harmful to bone health, particularly with adequate calcium intake. Dermal calcium losses might be an important consideration for endurance athletes, particularly during long training sessions or events. In these situations, some consideration should be given to pre-exercise calcium feeding. The avoidance of vitamin D deficiency and insufficiency is important for the athlete to protect their bone health. There remains a lack of information relating to the longer-term effects of different dietary and nutritional practices on bone health in athletes, something that needs to be addressed before specific guidance can be provided.

Published
2019
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21. Bone mineral density in high-level endurance runners: part A—site-specific characteristics

Author

Herbert, AJ, Williams, AG, Lockey, SJ, Erskine, RM, Sale, C, Hennis, PJ, Day, SH, Stebbings, GK, Herbert, AJ, Williams, AG, Lockey, SJ, Erskine, RM, Sale, C, Hennis, PJ, Day, SH, and Stebbings, GK

Abstract

Purpose Physical activity, particularly mechanical loading that results in high-peak force and is multi-directional in nature, increases bone mineral density (BMD). In athletes such as endurance runners, this association is more complex due to other factors such as low energy availability and menstrual dysfunction. Moreover, many studies of athletes have used small sample sizes and/or athletes of varying abilities, making it difficult to compare BMD phenotypes between studies. Method The primary aim of this study was to compare dual-energy X-ray absorptiometry (DXA) derived bone phenotypes of high-level endurance runners (58 women and 45 men) to non-athletes (60 women and 52 men). Our secondary aim was to examine the influence of menstrual irregularities and sporting activity completed during childhood on these bone phenotypes. Results Female runners had higher leg (4%) but not total body or lumbar spine BMD than female non-athletes. Male runners had lower lumbar spine (9%) but similar total and leg BMD compared to male non-athletes, suggesting that high levels of site-specific mechanical loading was advantageous for BMD in females only and a potential presence of reduced energy availability in males. Menstrual status in females and the number of sports completed in childhood in males and females had no influence on bone phenotypes within the runners. Conclusion Given the large variability in BMD in runners and non-athletes, other factors such as variation in genetic makeup alongside mechanical loading probably influence BMD across the adult lifespan.

Published
2021

22. The effects of short-term low energy availability, achieved through diet or exercise, on cognitive function in oral contraceptive users and eumenorrheic women

Author

Martin, D, Papageorgiou, M, Colgan, H, Bandelow, S, Greeves, JP, Tang, JCY, Fraser, WD, Cooper, SB, Sale, C, Elliott-Sale, K, Martin, D, Papageorgiou, M, Colgan, H, Bandelow, S, Greeves, JP, Tang, JCY, Fraser, WD, Cooper, SB, Sale, C, and Elliott-Sale, K

Abstract

To date, no research has explored the effects of low energy availability on cognitive performance using dietary and exercise regimens relevant to athletes. Twenty female participants (10 eumenorrheic, 10 oral contraceptive [OC] users) completed three 3-day conditions: 1) controlled-balanced energy availability without exercise (BAL; 45 kcal·kg lean body mass [LBM]1·day1); 2) diet-induced low energy availability without exercise (DIET; 15 kcal·kg LBM1·day 1); and 3) exercise-induced low energy availability (EX; 15 kcal·kg LBM1·day 1, including 30 kcal·kg LBM1·day 1 treadmill running at 70% maximal oxygen uptake). A cognitive test battery was completed before and after each 3-day condition. Mental rotation test accuracy improved in the BAL condition, but there was a decline in accuracy in the EX condition (BAL, +2.5%; EX, 1.4%; P = 0.042, d = 0.85). DIET (+1.3%) was not different to BAL or EX (P > 0.05). All other measures of cognitive performance were not affected by condition (P > 0.05) and OC use did not affect cognitive responses (P > 0.05). Accuracy in the mental rotation test was impaired when low energy availability was induced through increased exercise energy expenditure. All other aspects of cognition were unaffected by 3 days of low energy availability through diet or exercise. OC use did not mediate the effect of low energy availability on cognition. Novelty: Cognitive function was not affected by 3 days of diet-induced low energy availability. Only spatial awareness was impaired during 3 days of exercise-induced low energy availability. Reproductive hormones affected spatial awareness independent of energy availability.

Published
2021

23. The role of chronic muscle (in)activity on carnosine homeostasis: A study with spinal cord-injured athletes

Author

Nemezio, K, de Carvalho Yamaguchi, G, Boito Ramkrapes, AP, Schulz, ML, Baptista, IL, Riani, LA, Gonçalves, LDS, Sale, C, de Medeiros, MHG, Gualano, B, Artioli, GG, Nemezio, K, de Carvalho Yamaguchi, G, Boito Ramkrapes, AP, Schulz, ML, Baptista, IL, Riani, LA, Gonçalves, LDS, Sale, C, de Medeiros, MHG, Gualano, B, and Artioli, GG

Abstract

To examine the role of chronic (in)activity on muscle carnosine (MCarn) and how chronic (in)activity affects MCarn responses to b-alanine supplementation in spinal cord-injured athletes, 16 male athletes with paraplegia were randomized (2:1 ratio) to receive b-alanine (n = 11) or placebo (PL, n = 5). They consumed 6.4 g/day of b-alanine or PL for 28 days. Muscle biopsies of the active deltoid and the inactive vastus lateralis (VL) were taken before and after supplementation. MCarn in the VL was also compared with the VL of a group of individuals without paraplegia (n = 15). MCarn was quantified in whole muscle and in pools of individual fibers by high-performance liquid chromatography. MCarn was higher in chronically inactive VL vs. well-trained deltoid (32.0 ± 12.0 vs. 20.5 ± 6.1 mmol/kg DM; P = 0.018). MCarn was higher in inactive vs. active VL (32.0 ± 12.0 vs. 21.2 ± 7.5 mmol/kg DM; P = 0.011). In type-I fibers, MCarn was significantly higher in the inactive VL than in the active deltoid (38.3 ± 4.7 vs. 27.3 ± 11.8 mmol/kg DM, P = 0.014). MCarn increased similarly between inactive VL and active deltoid in the b-alanine group (VL: 68.9 ± 55.1%, P = 0.0002; deltoid: 90.5 ± 51.4%, P < 0.0001), with no changes in the PL group. MCarn content was higher in the inactive VL than in the active deltoid and the active VL, but this is probably a consequence of fiber type shift (type I to type II) that occurs with chronic inactivity. Chronically inactive muscle showed an increase in MCarn after BA supplementation equally to the active muscle, suggesting that carnosine accretion following b-alanine supplementation is not influenced by muscle inactivity.

Published
2021

24. A collagen extraction and deuterium oxide stable isotope tracer method for the quantification of bone collagen synthesis rates in vivo

Author

Civil, R, Brook, MS, Elliott-Sale, KJ, Santos, L, Varley, I, Lensu, S, Kainulainen, H, Koch, LG, Britton, SL, Wilkinson, DJ, Smith, K, Sale, C, Atherton, PJ, Civil, R, Brook, MS, Elliott-Sale, KJ, Santos, L, Varley, I, Lensu, S, Kainulainen, H, Koch, LG, Britton, SL, Wilkinson, DJ, Smith, K, Sale, C, and Atherton, PJ

Abstract

The development of safe and practical strategies to prevent weakening of bone tissue is vital, yet attempts to achieve this have been hindered by a lack of understanding of the short-term (days-weeks) physiology of bone collagen turnover. To address this, we have developed a method to quantify bone collagen synthesis in vivo, using deuterium oxide (D2O) tracer incorporation techniques combined with gas chromatography pyrolysis isotope-ratio mass spectrometry (GC-pyrolysis-IRMS). Forty-six male and female rats from a selectively bred model ingested D2O for 3 weeks. Femur diaphyses (FEM), tibia proximal (T-PRO), and distal (T-DIS) epiphyses-metaphyses and tibia mid-shaft diaphyses (T-MID) were obtained from all rats after necropsy. After demineralisation, collagen proteins were isolated and hydrolysed and collagen fractional synthetic rates (FSRs) determined by incorporation of deuterium into protein-bound alanine via GC-pyrolysis-IRMS. The collagen FSR for the FEM (0.131 ± 0.078%/day; 95% CI [0.106–0.156]) was greater than the FSR at T-MID (0.055 ± 0.049%/day; 95% CI [0.040–0.070]; p < 0.001). The T-PRO site had the highest FSR (0.203 ± 0.123%/day; 95% CI [0.166–0.241]) and T-DIS the lowest (0.027 ± 0.015%/day; 95% CI [0.022–0.031]). The three tibial sites exhibited different FSRs (p < 0.001). Herein, we have developed a sensitive method to quantify in vivo bone collagen synthesis and identified site-specific rates of synthesis, which could be applicable to studies of human bone collagen turnover.

Published
2021

25. Histidine dipeptides are key regulators of excitation-contraction coupling in cardiac muscle: evidence from a novel CARNS1 knockout rat model

Author

Gonçalves, LDS, Sales, LP, Saito, TR, Campos, JC, Fernandes, AL, Natali, J, Jensen, L, Arnold, A, Ramalho, L, Bechara, LRG, Esteca, MV, Correa, I, Sant'Anna, D, Ceroni, A, Michelini, LC, Gualano, B, Teodoro, W, Carvalho, VH, Vargas, BS, Medeiros, MHG, Baptista, IL, Irigoyen, MC, Sale, C, Ferreira, JCB, Artioli, GG, Gonçalves, LDS, Sales, LP, Saito, TR, Campos, JC, Fernandes, AL, Natali, J, Jensen, L, Arnold, A, Ramalho, L, Bechara, LRG, Esteca, MV, Correa, I, Sant'Anna, D, Ceroni, A, Michelini, LC, Gualano, B, Teodoro, W, Carvalho, VH, Vargas, BS, Medeiros, MHG, Baptista, IL, Irigoyen, MC, Sale, C, Ferreira, JCB, and Artioli, GG

Abstract

Histidine-containing dipeptides (HCDs) are abundantly expressed in striated muscles. Although important properties have been ascribed to HCDs, including H+ buffering, regulation of Ca2+ transients and protection against oxidative stress, it remains unknown whether they play relevant functions in vivo. To investigate the in vivo roles of HCDs, we developed the first carnosine synthase knockout (CARNS1−/−) rat strain to investigate the impact of an absence of HCDs on skeletal and cardiac muscle function. Male wild-type (WT) and knockout rats (4 months-old) were used. Skeletal muscle function was assessed by an exercise tolerance test, contractile function in situ and muscle buffering capacity in vitro. Cardiac function was assessed in vivo by echocardiography and cardiac electrical activity by electrocardiography. Cardiomyocyte contractile function was assessed in isolated cardiomyocytes by measuring sarcomere contractility, along with the determination of Ca2+ transient. Markers of oxidative stress, mitochondrial function and expression of proteins were also evaluated in cardiac muscle. Animals were supplemented with carnosine (1.8% in drinking water for 12 weeks) in an attempt to rescue tissue HCDs levels and function. CARNS1−/− resulted in the complete absence of carnosine and anserine, but it did not affect exercise capacity, skeletal muscle force production, fatigability or buffering capacity in vitro, indicating that these are not essential for pH regulation and function in skeletal muscle. In cardiac muscle, however, CARNS1−/− resulted in a significant impairment of contractile function, which was confirmed both in vivo and ex vivo in isolated sarcomeres. Impaired systolic and diastolic dysfunction were accompanied by reduced intracellular Ca2+ peaks and slowed Ca2+ removal, but not by increased markers of oxidative stress or impaired mitochondrial respiration. No relevant increases in muscle carnosine content were observed after carnosine supplementation. Resu

Published
2021

26. Atrophy Resistant vs. Atrophy Susceptible Skeletal Muscles: “aRaS” as a Novel Experimental Paradigm to Study the Mechanisms of Human Disuse Atrophy

Author

Bass, JJ, Hardy, EJO, Inns, TB, Wilkinson, DJ, Piasecki, M, Morris, RH, Spicer, A, Sale, C, Smith, K, Atherton, PJ, Phillips, BE, Bass, JJ, Hardy, EJO, Inns, TB, Wilkinson, DJ, Piasecki, M, Morris, RH, Spicer, A, Sale, C, Smith, K, Atherton, PJ, and Phillips, BE

Abstract

Objective: Disuse atrophy (DA) describes inactivity-induced skeletal muscle loss, through incompletely defined mechanisms. An intriguing observation is that individual muscles exhibit differing degrees of atrophy, despite exhibiting similar anatomical function/locations. We aimed to develop an innovative experimental paradigm to investigate Atrophy Resistant tibialis anterior (TA) and Atrophy Susceptible medial gastrocnemius (MG) muscles (aRaS) with a future view of uncovering central mechanisms. Method: Seven healthy young men (22 ± 1 year) underwent 15 days unilateral leg immobilisation (ULI). Participants had a single leg immobilised using a knee brace and air-boot to fix the leg (75° knee flexion) and ankle in place. Dual-energy X-ray absorptiometry (DXA), MRI and ultrasound scans of the lower leg were taken before and after the immobilisation period to determine changes in muscle mass. Techniques were developed for conchotome and microneedle TA/MG muscle biopsies following immobilisation (both limbs), and preliminary fibre typing analyses was conducted. Results: TA/MG muscles displayed comparable fibre type distribution of predominantly type I fibres (TA 67 ± 7%, MG 63 ± 5%). Following 15 days immobilisation, MG muscle volume (–2.8 ± 1.4%, p < 0.05) and muscle thickness decreased (−12.9 ± 1.6%, p < 0.01), with a positive correlation between changes in muscle volume and thickness (R2 = 0.31, p = 0.038). Importantly, both TA muscle volume and thickness remained unchanged. Conclusion: The use of this unique “aRaS” paradigm provides an effective and convenient means by which to study the mechanistic basis of divergent DA susceptibility in humans, which may facilitate new mechanistic insights, and by extension, mitigation of skeletal muscle atrophy during human DA.

Published
2021

27. Carnosine protects stimulus-secretion coupling through prevention of protein carbonyl adduction events in cells under metabolic stress

Author

Lavilla, CJ, Billacura, MP, Hanna, K, Boocock, DJ, Coveney, C, Miles, AK, Foulds, GA, Murphy, A, Tan, A, Jackisch, L, Sayers, SR, Caton, PW, Doig, CL, McTernan, PG, Colombo, SL, Sale, C, Turner, MD, Lavilla, CJ, Billacura, MP, Hanna, K, Boocock, DJ, Coveney, C, Miles, AK, Foulds, GA, Murphy, A, Tan, A, Jackisch, L, Sayers, SR, Caton, PW, Doig, CL, McTernan, PG, Colombo, SL, Sale, C, and Turner, MD

Abstract

Type 2 diabetes is characterised by failure to control glucose homeostasis, with numerous diabetic complications attributable to the resulting exposure of cells and tissues to chronic elevated concentrations of glucose and fatty acids. This, in part, results from formation of advanced glycation and advanced lipidation end-products that are able to modify protein, lipid, or DNA structure, and disrupt normal cellular function. Herein we used mass spectrometry to identify proteins modified by two such adduction events in serum of individuals with obesity, type 2 diabetes, and gestational diabetes, along with similar analyses of human and mouse skeletal muscle cells and mouse pancreatic islets exposed to glucolipotoxic stress. We also report that carnosine, a histidine containing dipeptide, prevented 65–90% of 4-hydroxynonenal and 3-nitrotyrosine adduction events, and that this in turn preserved mitochondrial function and protected stimulus-secretion coupling in cells exposed to metabolic stress. Carnosine therefore offers significant therapeutic potential against metabolic diseases.

Published
2021

28. Effect of menstrual cycle phase, menstrual irregularities and hormonal contraceptive use on anterior knee laxity and non-contact anterior cruciate ligament injury occurrence in women: A protocol for a systematic review and meta-analysis

Author

Nédélec, E, Foli, E, Shultz, SJ, Swinton, PA, Dolan, E, Enright, K, Piasecki, J, Matthews, JJ, Sale, C, Elliott-Sale, KJ, Nédélec, E, Foli, E, Shultz, SJ, Swinton, PA, Dolan, E, Enright, K, Piasecki, J, Matthews, JJ, Sale, C, and Elliott-Sale, KJ

Abstract

Exercising women report three to six times more ACL tears than men, which happen, in the majority of cases, with a non-contact mechanism. This sex disparity has, in part, been attributed to the differences in reproductive hormone profiles between men and women. Many studies have shown that anterior knee (AK) laxity and the rate of non-contact ACL injuries vary across the menstrual cycle, but these data are inconsistent. Similarly, several studies have investigated the potential protective effect of hormonal contraceptives on non-contact ACL injuries, but their conclusions are also variable. The purpose of this systematic review and meta-analysis is to, identify, evaluate and summarise the effects of endogenous and exogenous ovarian hormones on AK laxity (primary outcome) and the occurrence of non-contact ACL injuries (secondary outcome) in women. We will perform a systematic search for all observational studies conducted on this topic. Studies will be retrieved by searching electronic databases, clinical trial registers, author’s personal files and cross-referencing selected studies. Risk of bias will be assessed using the Newcastle Ottawa Quality Assessment Scale for Cohort and Case–Control Studies. Certainty in the cumulative evidence will be assessed using the Grading of Recommendations Assessment, Development and Evaluation approach. The meta-analyses will use a Bayesian approach to address specific research questions in a more intuitive and probabilistic manner. This review is registered on the international database of prospectively registered systematic reviews (PROSPERO; CRD42021252365).

Published
2021

33. Period Prevalence and Perceived Side Effects of Hormonal Contraceptive Use and the Menstrual Cycle in Elite Athletes

Author

Martin, D, Sale, C, Cooper, SB, and Elliott-Sale, KJ

Subjects
Adult, medicine.medical_specialty, media_common.quotation_subject, Emotions, Prevalence, Physical Therapy, Sports Therapy and Rehabilitation, Contraceptives, Oral, Hormonal, Injections, Menstruation, Young Adult, 03 medical and health sciences, 0302 clinical medicine, Surveys and Questionnaires, medicine, Humans, Orthopedics and Sports Medicine, Elite athletes, Menstrual Cycle, Menstruation Disturbances, Menstrual cycle, media_common, Drug Implants, 030219 obstetrics & reproductive medicine, biology, Athletes, Obstetrics, business.industry, Intrauterine Devices, Medicated, C600 Sports Science, 030229 sport sciences, biology.organism_classification, Discontinuation, Contraceptives, Oral, Combined, Contraceptive use, Female, Perception, Progestins, business, Hormone
Abstract

Purpose:To identify the period prevalence of hormonal contraceptive (HC) use and characterize the perceived side effects associated with the menstrual cycle and HC use.Methods:A total of 430 elite female athletes completed a questionnaire to assess the period prevalence of HC use, the reasons for initiation and discontinuation of HCs, and the side effects experienced by HC and non-HC users. Descriptive statistics, between-groups comparisons, and associations between categorical variables were calculated.Results:Of athletes studied, 49.5% were currently using HCs and 69.8% had used HCs at some point. Combined oral contraceptives were most commonly used (68.1%), with 30.0% using progestin-only contraceptives (implant = 13.1%, injection = 3.7%, and intrauterine system = 2.8%). Perceived negative side effects were more common with progestin-only HC use (39.1%) compared with combined-HC use (17.8%;P = .001) and were most prevalent in implant users (53.6%;P = .004). HC users reported perceived positive side effects relating to their ability to predict and/or manipulate the timing, frequency, and amount of menstrual bleeding. Non-HC users had a menstrual cycle length of 29 (5) d and 77.4% reported negative side effects during their menstrual cycle, primarily during days 1–2 of menstruation (81.6%).Conclusions:Approximately half of elite athletes used HCs, and progestin-only contraceptive users reported greater incidences of negative side effects, especially with the implant. Because of the high interindividual variability in reported side effects, athletes and practitioners should maintain an open dialogue to pursue the best interests of the athlete.

Published
2018
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35. Exercise and bone health across the lifespan

Author

Santos, L, Elliott-Sale, KJ, and Sale, C

Subjects
0301 basic medicine, Peak bone mass, Aging, medicine.medical_specialty, Anabolism, Osteoporosis, 030209 endocrinology & metabolism, Bone tissue, Bioinformatics, Bone and Bones, Bone health, 03 medical and health sciences, Absorptiometry, Photon, Life Expectancy, 0302 clinical medicine, Internal medicine, Bone cell, medicine, Humans, Bone adaptation, Epigenetics, Exercise, Lifespan, business.industry, medicine.disease, Adaptation, Physiological, Menopause, 030104 developmental biology, medicine.anatomical_structure, Endocrinology, Ageing, Bone Remodeling, Geriatrics and Gerontology, business, Bone ageing, Gerontology, Research Article
Abstract

With ageing, bone tissue undergoes significant compositional, architectural and metabolic alterations potentially leading to osteoporosis. Osteoporosis is the most prevalent bone disorder, which is characterised by progressive bone weakening and an increased risk of fragility fractures. Although this metabolic disease is conventionally associated with ageing and menopause, the predisposing factors are thought to be established during childhood and adolescence. In light of this, exercise interventions implemented during maturation are likely to be highly beneficial as part of a long-term strategy to maximise peak bone mass and hence delay the onset of age- or menopause-related osteoporosis. This notion is supported by data on exercise interventions implemented during childhood and adolescence, which confirmed that weight-bearing activity, particularly if undertaken during peripubertal development, is capable of generating a significant osteogenic response leading to bone anabolism. Recent work on human ageing and epigenetics suggests that undertaking exercise after the fourth decade of life is still important, given the anti-ageing effect and health benefits provided, potentially occurring via a delay in telomere shortening and modification of DNA methylation patterns associated with ageing. Exercise is among the primary modifiable factors capable of influencing bone health by preserving bone mass and strength, preventing the death of bone cells and anti-ageing action provided.

Published
2017
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41. The effects of short-term low energy availability, achieved through diet or exercise, on cognitive function in oral contraceptive users and eumenorrheic women.

Author

Martin, D., Papageorgiou, M., Colgan, H., Bandelow, S., Greeves, J.P., Tang, J.C.Y., Fraser, W.D., Cooper, S.B., Sale, C., and Elliott-Sale, K.J.

Subjects
ENERGY metabolism, MENSTRUAL cycle, INGESTION, DIET, ORAL contraceptives, EXERCISE, DESCRIPTIVE statistics, COGNITIVE testing, SPACE perception
Abstract

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Published
2021
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42. A medieval garden at the Belgrave moat, Cheshire

Author

Turner, R C, Sale, C B, and Rutter, Janet A

Abstract

Journal of the Chester Archaeological Society, 69, 59-77, Detailed survey, with trial dig, of a complex site and its environs; historical evidence suggests its owner as a royal servant, Richard the Engineer (of Edward I).

Published
2018
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43. The interactions of physical activity, exercise and genetics and their associations with bone mineral density: implications for injury risk in elite athletes

Author

Herbert, AJ, Williams, AG, Hennis, PJ, Erskine, RM, Sale, C, Day, SH, Stebbings, GK, Herbert, AJ, Williams, AG, Hennis, PJ, Erskine, RM, Sale, C, Day, SH, and Stebbings, GK

Abstract

Low bone mineral density (BMD) is established as a primary predictor of osteoporotic risk and can also have substantial implications for athlete health and injury risk in the elite sporting environment. BMD is a highly multi-factorial phenotype influenced by diet, hormonal characteristics and physical activity. The interrelationships between such factors, and a strong genetic component, suggested to be around 50–85% at various anatomical sites, determine skeletal health throughout life. Genome-wide association studies and case–control designs have revealed many loci associated with variation in BMD. However, a number of the candidate genes identified at these loci have no known associated biological function or have yet to be replicated in subsequent investigations. Furthermore, few investigations have considered gene–environment interactions—in particular, whether specific genes may be sensitive to mechanical loading from physical activity and the outcome of such an interaction for BMD and potential injury risk. Therefore, this review considers the importance of physical activity on BMD, genetic associations with BMD and how subsequent investigation requires consideration of the interaction between these determinants. Future research using well-defined independent cohorts such as elite athletes, who experience much greater mechanical stress than most, to study such phenotypes, can provide a greater understanding of these factors as well as the biological underpinnings of such a physiologically “extreme” population. Subsequently, modification of training, exercise or rehabilitation programmes based on genetic characteristics could have substantial implications in both the sporting and public health domains once the fundamental research has been conducted successfully.

Published
2018

44. A Comparative Study of Hummingbirds and Chickens Provides Mechanistic Insight on the Histidine Containing Dipeptide Role in Skeletal Muscle Metabolism

Author

Dolan, E, Saunders, B, Dantas, W, Murai, I H, Roschel, H, Artioli, G, Harris, R, Bicudo, Jose E, Sale, C, Gualano, B, Dolan, E, Saunders, B, Dantas, W, Murai, I H, Roschel, H, Artioli, G, Harris, R, Bicudo, Jose E, Sale, C, and Gualano, B

Abstract

Histidine containing dipeptides (HCDs) have numerous ergogenic and therapeutic properties, but their primary role in skeletal muscle remains unclear. Potential functions include pH regulation, protection against reactive oxygen/nitrogen species, or Ca2+regulation. In recognition of the challenge of isolating physiological processes in-vivo, we employed a comparative physiology approach to investigate the primary mechanism of HCD action in skeletal muscle. We selected two avian species (i.e., hummingbirds and chickens), who represented the extremes of the physiological processes in which HCDs are likely to function. Our findings indicate that HCDs are non-essential to the development of highly oxidative and contractile muscle, given their very low content in hummingbird skeletal tissue. In contrast, their abundance in the glycolytic chicken muscle, indicate that they are important in anaerobic bioenergetics as pH regulators. This evidence provides new insights on the HCD role in skeletal muscle, which could inform widespread interventions, from health to elite performance.

Published
2018

45. Large-scale GWAS identifies multiple loci for hand grip strength providing biological insights into muscular fitness

Author

Willems, SM, Wright, DJ, Day, FR, Trajanoska, K, Joshi, PK, Morris, JA, Matteini, AM, Garton, FC, Grarup, N, Oskolkov, N, Thalamuthu, A, Mangino, M, Liu, J, Demirkan, A, Lek, M, Xu, L, Wang, G, Oldmeadow, C, Gaulton, KJ, Lotta, LA, Miyamoto-Mikami, E, Rivas, MA, White, T, Loh, P-R, Aadahl, M, Amin, N, Attia, JR, Austin, K, Benyamin, B, Brage, S, Cheng, Y-C, Cięszczyk, P, Derave, W, Eriksson, K-F, Eynon, N, Linneberg, A, Lucia, A, Massidda, M, Mitchell, BD, Miyachi, M, Murakami, H, Padmanabhan, S, Pandey, A, Papadimitriou, I, Rajpal, DK, Sale, C, Schnurr, TM, Sessa, F, Shrine, N, Tobin, MD, Varley, I, Wain, LV, Wray, NR, Lindgren, CM, MacArthur, DG, Waterworth, DM, McCarthy, MI, Pedersen, O, Khaw, K-T, Kiel, DP, Oei, L, Zheng, H-F, Forgetta, V, Leong, A, Ahmad, OS, Laurin, C, Mokry, LE, Ross, S, Elks, CE, Bowden, J, Warrington, NM, Murray, A, Ruth, KS, Tsilidis, KK, Medina-Gómez, C, Estrada, K, Bis, JC, Chasman, DI, Demissie, S, Enneman, AW, Hsu, Y-H, Ingvarsson, T, Kähönen, M, Kammerer, C, Lacroix, AZ, Li, G, Liu, C-T, Liu, Y, Lorentzon, M, Mägi, R, Mihailov, E, Milani, L, Moayyeri, A, Nielson, CM, Sham, PC, Siggeirsdotir, K, Sigurdsson, G, Stefansson, K, Trompet, S, Thorleifsson, G, Vandenput, L, van der Velde, N, Viikari, J, Xiao, S-M, Zhao, JH, Evans, DS, Cummings, SR, Cauley, J, Duncan, EL, de Groot, LCPGM, Esko, T, Gudnason, V, Harris, TB, Jackson, RD, Jukema, JW, Ikram, AMA, Karasik, D, Kaptoge, S, Kung, AWC, Lehtimäki, T, Lyytikäinen, L-P, Lips, P, Luben, R, Metspalu, A, van Meurs, JBJ, Minster, RL, Orwoll, E, Oei, E, Psaty, BM, Raitakari, OT, Ralston, SW, Ridker, PM, Robbins, JA, Smith, AV, Styrkarsdottir, U, Tranah, GJ, Thorstensdottir, U, Uitterlinden, AG, Zmuda, J, Zillikens, MC, Ntzani, EE, Evangelou, E, Ioannidis, JPA, Evans, DM, Ohlsson, C, Pitsiladis, Y, Fuku, N, Franks, PW, North, KN, van Duijn, CM, Mather, KA, Hansen, T, Hansson, O, Spector, T, Murabito, JM, Richards, JB, Rivadeneira, F, Langenberg, C, Perry, JRB, Wareham, NJ, Scott, RA, Willems, Sara M, Wright, Daniel J, Day, Felix R, Trajanoska, Katerina, Benyamin, Beben, Scott, Robert A, GEFOS Anytype Fracture Consortium, Wright, Daniel [0000-0003-3983-2093], Day, Felix [0000-0003-3789-7651], White, Thomas [0000-0001-8456-0803], Brage, Soren [0000-0002-1265-7355], Khaw, Kay-Tee [0000-0002-8802-2903], Langenberg, Claudia [0000-0002-5017-7344], Perry, John [0000-0001-6483-3771], Wareham, Nicholas [0000-0003-1422-2993], Apollo - University of Cambridge Repository, Epidemiology, and Internal Medicine

Subjects
Male, Genome-wide association study, VARIANTS, Physical strength, DISEASE, Grip strength, 0302 clinical medicine, Neoplasm Proteins/genetics, GENETIC INFLUENCES, European Continental Ancestry Group/genetics, Aetiology, education.field_of_study, Hand Strength, Deporte, 3. Good health, Neoplasm Proteins, muscular fitness, Science & Technology - Other Topics, Medical genetics, medicine.medical_specialty, Science, 1.1 Normal biological development and functioning, European Continental Ancestry Group, ta3111, Article, White People, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, FRACTURES, Genetics, Humans, GENOME-WIDE ASSOCIATION, Genetik, Polymorphism, education, METAANALYSIS, Aged, VLAG, Global Nutrition, Wereldvoeding, Science & Technology, ta1184, Prevention, Hand/physiology, Biology and Life Sciences, INSTRUMENTS, Hand, GEFOS Any-Type of Fracture Consortium, Nuclear Proteins/genetics, Genetics, Population, 030104 developmental biology, Genetic Loci, 030217 neurology & neurosurgery, 0301 basic medicine, Transforming Growth Factor alpha/genetics, General Physics and Astronomy, Bioinformatics, GROWTH-FACTOR-ALPHA, Cohort Studies, Medicine and Health Sciences, 2.1 Biological and endogenous factors, ta315, Multidisciplinary, Nuclear Proteins, Single Nucleotide, Middle Aged, Multidisciplinary Sciences, MENDELIAN RANDOMIZATION, SKELETAL-MUSCLE, Female, Medical Genetics, Adult, Population, Quantitative trait locus, Biology, Polymorphism, Single Nucleotide, Underpinning research, Hand strength, MD Multidisciplinary, Mendelian randomization, medicine, Life Science, Membrane Proteins/genetics, Deportes, Medicinsk genetik, Repressor Proteins/genetics, Whites, Actins/genetics, Membrane Proteins, General Chemistry, Transforming Growth Factor alpha, Genética, Actins, United Kingdom, Repressor Proteins, Good Health and Well Being, Exercise Physiology and nutrition, Musculoskeletal, genome-wide association, Genome-Wide Association Study
Abstract

Hand grip strength is a widely used proxy of muscular fitness, a marker of frailty, and predictor of a range of morbidities and all-cause mortality. To investigate the genetic determinants of variation in grip strength, we perform a large-scale genetic discovery analysis in a combined sample of 195,180 individuals and identify 16 loci associated with grip strength (P, Hand grip strength as a proxy of muscular fitness is a clinical predictor of mortality and morbidity. In a large-scale GWA study, the authors find 16 robustly associated genetic loci that highlight roles in muscle fibre structure and function, neuronal maintenance and nervous system signal transduction.

Published
2017
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46. Associations of bone mineral density-related genes and marathon performance in elite European Caucasian marathon runners.

Author

Herbert, AJ, Williams, AG, Lockey, SJ, Erskine, RM, Hennis, PJ, Sale, C, Day, SH, Stebbings, GK, Herbert, AJ, Williams, AG, Lockey, SJ, Erskine, RM, Hennis, PJ, Sale, C, Day, SH, and Stebbings, GK

Abstract

Bone mineral density (BMD) is a multi-factorial phenotype determined by factors such as physical activity, diet and a sizeable genetic component. Athletic populations tend to possess higher BMD than non-athletes due to a larger volume of exercise completed. Despite this, some endurance runners can possess low BMD and/or suffer stress fractures, which can have negative impacts on their health and performance. Therefore, we hypothesised that elite endurance runners would possess a genotype associated with enhanced BMD and a reduced risk of injury, resulting in less training interruption and greater potential success. The study compared the genotype and allele frequencies of 5 genetic variants associated with BMD (LRP5 rs3736228, TNFRSF11B rs4355801, VDR rs2228570, WNT16 rs3801387, AXIN1 rs9921222) in elite (men < 2 h 30 min, n = 110; women < 3 h 00 min, n = 98) and sub-elite (men 2 h 30 min – 2 h 45 min, n = 181; women 3 h 00 min – 3 h 15 min, n = 67) marathon runners with those of a non-athlete control population (n = 474). We also investigated whether marathon personal best time was associated with a more “advantageous” BMD genotype. Congruent with our hypothesis, the “risk” T allele for the AXIN1 rs9921222 polymorphism was 5% more frequent in the control group than in sub-elites (P = 0.030, χ2 = 4.69) but no further differences were observed for this variant (P ≥ 0.083, χ2 ≤ 4.98). WNT16 rs3801387 genotype frequency differed between athletes and controls (P = 0.002, χ2 = 12.02) and elites vs controls (P = 0.008, χ2 = 9.72), as did allele frequency. However, contrary to our hypothesis, it was the “risk” A allele that was ~5% more frequent in athletes than controls. Similarly, when combining data from all 5 variants, the athletes had a lower Total Genotype Score than controls (53.6 vs 65.7; P ≤ 0.001), again suggesting greater genetic susceptibility to bone injury in athletes. Personal best times were not associated with genotype in any comparison. These results sugg

Published
2017

47. Athlome project consortium: A concerted effort to discover genomic and other 'omic' markers of athletic performance

Author

Pitsiladis, Y.P. Tanaka, M. Eynon, N. Bouchard, C. North, K.N. Williams, A.G. Collins, M. Moran, C.N. Britton, S.L. Fuku, N. Ashley, E.A. Klissouras, V. Lucia, A. Ahmetov, I.I. De Geus, E. Alsayrafi, M. Webborn, N. Wang, G. Bishop, D.J. Papadimitriou, I. Yan, X. Tirosh, O. Kuang, J. Rankinen, T. Sarzinsky, M. Mikael Mattsson, C. Wheeler, M. Waggott, D. Byrne, N.M. Artioli, G.G. September, A. Posthumus, M. Van der Merwe, W. Cieszczyk, P. Leonska-Duniec, A. Ficek, K. Maciejewska-Karlowska, A. Sawczuk, M. Stepien-Slodkowska, M. Feller, J. Dijkstra, P. Chmutov, A.M. Dyatlov, D.A. Orekhov, E.F. Pushkareva, Y.E. Shvedkaya, I.A. Massidda, M. Calò, C.M. Day, S.H. Stebbings, G.K. Erskine, R.M. Montgomery, H.E. Garton, F.C. Houweling, P. Derave, W. Baguet, A. Muniesa, C.A. Sessa, F. Petito, A. Sale, C. Hughes, D.C. Varley, I. Boomsma, D. Bartels, M. Davies, G.E. Ginevičienė, V. Jakaitienė, A. Kučinskas, V. Tubelis, L. Utkus, A. Milašius, K. Venckunas, T. Skurvydas, A. Stasiulis, A. Malkova, D. Wilson, R. Koch, L.G. Zempo, H. Naito, H. Kikuchi, N. Miyamoto-Mikami, E. Murakami, H. Miyachi, M. Takahashi, H. Ohiwa, N. Kawahara, T. Tsuchie, H. Tobina, T. Ichinoseki-Sekine, N. Tanaka, H. Kaneoka, K. Nakazato, K. Egorova, E.S. Gabdrakhmanova, L.J. Arkhipova, A.A. Borisova, A.V. Gabbasov, R.T. Stepanova, A.A. Kashapov, R.I. Rogozkin, V.A. Astratenkova, I.V. Druzhevskaya, A.M. Fedotovskaya, O.N. Golberg, N.D. Hakimullina, A.M. Kostryukova, E.S. Alexeev, D.G. Generozov, E.V. Ischenko, D.S. Kulemin, N.A. Larin, A.K. Ospanova, E.A. Pavlenko, A.V. Govorun, V.M. Gilep, A.A. Gilep, I.L. Haidukevich, I.V. Rybina, I.L. Drozdovska, S.B. Docenko, V.E. Ilyin, V.N. Lekontsev, E. Akimov, E.B. El-Rayess, M. Georgakopoulos, C. Botre, F. Suhre, K. Hubank, M. Wolfarth, B. Greeves, J.P. Stellingwerff, T. Ranson, C. Fraser, W.D. Grealy, R. Griffiths, L. Scott, R. Pushkarev, V.P. Athlome Project Consortium

Abstract

Despite numerous attempts to discover genetic variants associated with elite athletic performance, injury predisposition, and elite/world-class athletic status, there has been limited progress to date. Past reliance on candidate gene studies predominantly focusing on genotyping a limited number of single nucleotide polymorphisms or the insertion/deletion variants in small, often heterogeneous cohorts (i.e., made up of athletes of quite different sport specialties) have not generated the kind of results that could offer solid opportunities to bridge the gap between basic research in exercise sciences and deliverables in biomedicine. A retrospective view of genetic association studies with complex disease traits indicates that transition to hypothesis-free genome-wide approaches will be more fruitful. In studies of complex disease, it is well recognized that the magnitude of genetic association is often smaller than initially anticipated, and, as such, large sample sizes are required to identify the gene effects robustly. A symposium was held in Athens and on the Greek island of Santorini from 14 -17 May 2015 to review the main findings in exercise genetics and genomics and to explore promising trends and possibilities. The symposium also offered a forum for the development of a position stand (the Santorini Declaration). Among the participants, many were involved in ongoing collaborative studies (e.g., ELITE, GAMES, Gene SMART, GENESIS, and POWERGENE). A consensus emerged among participants that it would be advantageous to bring together all current studies and those recently launched into one new large collaborative initiative, which was subsequently named the Athlome Project Consortium. © 2016 the American Physiological Society.

Published
2016

48. The Athlome Project Consortium: A Concerted Effort to Discover Genomic and other 'OMIC' Markers of Athletic Performance

Author

Pitsiladis, Y. P., Tanaka, M., Eynon, N., Bouchard, C., North, K. N., Williams, A. G., Collins, M., Moran, C. N., Britton, S. L., Fuku, N., Ashley, E. A., Klissouras, V., Lucia, A., Ahmetov, I. I., De Geus, E., Alsayrafi, M., Webborn, N., Wang, G., Bishop, D. J., Papadimitriou, I., Yan, X., Tirosh, O., Kuang, J., Rankinen, T., Sarzinsky, M., Mikael Mattsson, C., Wheeler, M., Waggott, D., Byrne, N. M., Artioli, G. G., September, A., Posthumus, M., Van der Merwe, W., Cieszczyk, P., Leonska-Duniec, A., Ficek, K., Maciejewska-Karlowska, A., Sawczuk, M., Stepien-Slodkowska, M., Feller, J., Dijkstra, P., Chmutov, A. M., Dyatlov, D. A., Orekhov, E. F., Pushkareva, Y. E., Shvedkaya, I. A., Massidda, M., Calo, C. M., Day, S. H., Stebbings, G. K., Erskine, R. M., Montgomery, H. E., Garton, F. C., Houweling, P., Derave, W., Baguet, A., Muniesa, C. A., Sessa, F., Petito, A., Sale, C., Hughes, D. C., Varley, I., Boomsma, D., Bartels, M., Davies, G. E., Gineviciene, V., Jakaitiene, A., Kucinskas, V., Tubelis, L., Utkus, A., Milasius, K., Venckunas, T., Skurvydas, A., Stasiulis, A., Malkova, D., Wilson, R., Koch, L. G., Zempo, H., Naito, H., Kikuchi, N., Miyamoto-Mikami, E., Murakami, H., Miyachi, M., Takahashi, H., Ohiwa, N., Kawahara, T., Tsuchie, H., Tobina, T., Ichinoseki-Sekine, N., Tanaka, H., Kaneoka, K., Nakazato, K., Egorova, E. S., Gabdrakhmanova, L. J., Arkhipova, A. A., Borisova, A. V., Gabbasov, R. T., Stepanova, A. A., Kashapov, R. I., Rogozkin, V. A., Astratenkova, I. V., Druzhevskaya, A. M., Fedotovskaya, O. N., Golberg, N. D., Hakimullina, A. M., Kostryukova, E. S., Alexeev, D. G., Generozov, E. V., Ischenko, D. S., Kulemin, N. A., Larin, A. K., Ospanova, E. A., Pavlenko, A. V., Govorun, V. M., Gilep, A. A., Gilep, I. L., Haidukevich, I. V., Rybina, I. L., Drozdovska, S. B., Docenko, V. E., Ilyin, V. N., Lekontsev, E., Akimov, E. B., El-Rayess, M., Georgakopoulos, C., Botre, F., Suhre, K., Hubank, M., Wolfarth, B., Greeves, J. P., Stellingwerff, T., Ranson, C., Fraser, W. D., Grealy, R., Griffiths, L., Scott, R., Pushkarev, V. P., Biological Psychology, EMGO+ - Lifestyle, Overweight and Diabetes, and Amsterdam Neuroscience - Mood, Anxiety, Psychosis, Stress & Sleep

Subjects
0301 basic medicine, Candidate gene, Physiology, Sports genomics, Performance, Declaration, Genomics, Tissue Banks, Athletic Performance, Genética humana, Epigenesis, Genetic, RC1200, 03 medical and health sciences, 0302 clinical medicine, SDG 17 - Partnerships for the Goals, Genetic, Atleta, Genetics, Animals, Humans, QH426, Biomedicine, Genetic association, Atletismo, biology, Athletes, business.industry, Call for Papers: Systems Biology and Polygenic Traits, 030229 sport sciences, Atletas, Deporte, biology.organism_classification, QP, Data science, Biobank, Europe, 030104 developmental biology, Elite, business, Biomarkers, Epigenesis
Abstract

Despite numerous attempts to discover genetic variants associated with elite athletic performance, injury predisposition and elite/world-class athletic status, there has been limited progress to date. Past reliance on candidate gene studies predominantly focusing on genotyping a limited number of single nucleotide polymorphisms (SNPs) or the insertion/deletion variants in small, often heterogeneous cohorts have not generated the kind of results that could offer solid opportunities to bridge the gap between basic research in exercise sciences and deliverables in biomedicine. A retrospective view of genetic association studies with complex disease traits indicates that transition to hypothesis-free genome-wide approaches will be more fruitful. In studies of complex disease, it is well recognized that the magnitude of genetic associations is often smaller than initially anticipated and, as such, large sample sizes are required to identify them robustly. Thus, alternative approaches involving large-scale, collaborative efforts, within which high-resolution genome-wide data is generated and interrogated using advanced bioinformatics approaches, are likely necessary for meaningful progress to be made. Accordingly, a symposium was held on the Greek island of Santorini from 14-17th May 2015 to review the main findings in exercise genetics and genomics and to explore promising trends and possibilities. The symposium offered a forum for the development of a position stand. Among the participants, many were involved in ongoing collaborative studies. A consensus emerged among participants that it would be advantageous to bring together all current studies and those recently launched into one new large collaborative initiative, which was subsequently named the Athlome Project Consortium. Sin financiación 3.044 JCR (2016) Q2, 26/84 Physiology, 68/167 Genetics and Heredity; Q3, 104/190 Cell Biology 1.448 SJR (2016) Q2, 106/351 Genetics, 47/191 Physiology No data IDR 2016 UEM

Published
2016
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