Sex differences in survival and mitochondrial bioenergetics during aging in<i>Drosophila</i>

Ballard, J. William O.; Melvin, Richard G; Miller, Joseph T.; Katewa, Subhash D.

doi:10.1111/j.1474-9726.2007.00331.x

Cited by 50 publications

(46 citation statements)

References 75 publications

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“…Only male flies showed positive association between enzymatic activities and transcript levels of SOD and catalase which may indicate tight regulation of these enzymes on transcriptional level. Similar sex-specificity of antioxidant response was observed in previous studies (Ballard et al, 2007;Lushchak et al, 2011;Lozinsky et al, 2012Lozinsky et al, , 2013. Strong dependence of catalase activity on fly gender might be explained by different expression of catalase isoforms (CG6871 and CG9314) in males and females.…”

Section: Sex-specific Metabolic and Antioxidant Response To Dietary Ssupporting

confidence: 79%

High sucrose consumption promotes obesity whereas its low consumption induces oxidative stress in Drosophila melanogaster

Rovenko

Kubrak

Gospodaryov

et al. 2015

Journal of Insect Physiology

101

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Section: Sex-specific Metabolic and Antioxidant Response To Dietary Ssupporting

confidence: 79%

High sucrose consumption promotes obesity whereas its low consumption induces oxidative stress in Drosophila melanogaster

Rovenko

Kubrak

Gospodaryov

et al. 2015

Journal of Insect Physiology

101

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“…Although the mother's curse hypothesis has enjoyed experimental support [36], and mtDNA mutations are likely to increase variance in male aging, neither of these two hypotheses is likely to provide a general explanation for the evolution of sex differences in longevity and aging because males live longer than females in many taxa [7,12,37,38]. Our results show that selection on males, and in a broad sense, sex-limited selection in either sex, is sufficient to generate sexual dimorphism in aging and longevity, whereas the interaction between the rate and the source of mortality (i.e., whether mortality is random or condition dependent, with respect to whole-organism performance) can determine which sex will live the longest.…”

Section: Resultsmentioning

confidence: 99%

Condition Dependence of Male Mortality Drives the Evolution of Sex Differences in Longevity

Chen

Maklakov

2014

Current Biology

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Males and females age at different rates and have different life expectancies across the animal kingdom, but what causes the longevity "gender gaps" remains one of the most fiercely debated puzzles among biologists and demographers. Classic theory predicts that the sex experiencing higher rate of extrinsic mortality evolves faster aging and reduced longevity. However, condition dependence of mortality can counter this effect by selecting against senescence in whole-organism performance. Contrary to the prevailing view but in line with an emerging new theory, we show that the evolution of sex difference in longevity depends on the factors that cause sex-specific mortality and cannot be predicted from the mortality rate alone. Experimental evolution in an obligately sexual roundworm, Caenorhabditis remanei, in which males live longer than females, reveals that sexual dimorphism in longevity erodes rapidly when the extrinsic mortality in males is increased at random. We thus experimentally demonstrate evolution of the sexual monomorphism in longevity in a sexually dimorphic organism. Strikingly, when extrinsic mortality is increased in a way that favors survival of fast-moving individuals, males evolve increased longevities, thereby widening the gender gap. Thus, sex-specific selection on whole-organism performance in males renders them less prone to the ravages of old age than females, despite higher rates of extrinsic mortality. Our results reconcile previous research with recent theoretical breakthroughs by showing that sexual dimorphism in longevity evolves rapidly and predictably as a result of the sex-specific interactions between environmental hazard and organism's condition.

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“…Age and sex were reported as two confounding factors related to alteration of the mtDNA copy number 5,11) .Then we applied the partial correlation to process the analysis in Table 2 under age and sex control. MtDNA copy number of leukocytes from subjects with MetS was found to correlate positively with the HDL-cholesterol concentration and negatively with blood pressure, HOMA-IR and triglyceride concentration; however, the mtDNA copy number was not significantly correlated with waist circumference, smoking index, fasting glucose, insulin, BUN, creatinine, total cholesterol, or LDL-cholesterol concentration.…”

Section: Resultsmentioning

confidence: 99%

Depleted Leukocyte Mitochondrial DNA Copy Number in Metabolic Syndrome

Huang

Hsieh

et al. 2011

JAT

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Sex differences in survival and mitochondrial bioenergetics during aging inDrosophila

Cited by 50 publications

References 75 publications

High sucrose consumption promotes obesity whereas its low consumption induces oxidative stress in Drosophila melanogaster

High sucrose consumption promotes obesity whereas its low consumption induces oxidative stress in Drosophila melanogaster

Condition Dependence of Male Mortality Drives the Evolution of Sex Differences in Longevity

Depleted Leukocyte Mitochondrial DNA Copy Number in Metabolic Syndrome

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