What makes individuals attractive and why do we have the preferences that we do? Effective indicators of sexual attractiveness must be an honest reflection of an individual's health and reproductive potential and as such, must be linked at the molecular level to the key fitness parameters that they represent. However, very few studies have identified specific molecular relationships that link attractive traits to the pathways that influence reproductive fitness. Our preliminary data establish that: (i) both aging and the insulin signaling pathway modulate the production of specific chemical pheromones in Drosophila (a.ka., cuticular hydrocarbons) through transcriptional regulation of key enzymes involved in hydrocarbon synthesis, (ii) that these changes cause alterations in animal sexual attractiveness, and (iii) mechanisms underlying these effects may also involve a second nutrient-sensing pathway, the TOR pathway. Based on these data, we hypothesize that certain attractive traits may represent conspicuous extensions of molecular pathways that are critical for determining fitness. We will test this hypothesis by dissecting the immediate molecular links between insulin signaling and TOR activity, pheromone composition, reproductive function, and sexual attractiveness in Drosophila. We will also investigate the impact of these links on genetic variation in natural populations. This work is important because an understanding of molecular links leading from genotype to attractiveness, and the selective forces acting on them, would open the door for a more detailed analysis of the evolution of mate choice and provide insight into mechanisms underlying the physiological constraints that drive trait evolution. Our approach is innovative because it combines targeted genetic manipulations with measures of behavior to identify molecular underpinnings of links between mate quality, nutrient-sensing, and sexual attractiveness. We will then ask whether these mechanisms can also account for natural variation. In other words, we will be able to assess the extent to which what we discover in the lab is relevant in the field. Our research will further our understanding of two important nutrient sensing pathways that are implicated in many human illnesses, including cancer, diabetes and heart disease. Furthermore, these studies may reveal molecular signatures of metabolic pathways that can be used as indicators in early diagnosis of disease, and they may foreshadow the development of accurate and cheap early detection of disease by chemosensory methods.

Public Health Relevance

Studies have shown that organisms respond to cues that indicate metabolic and disease pathway activity in their potential mates or rivals, but the molecular basis for the connection between individual cues and pathway activity is unknown. Here we focus on the influence that two major evolutionarily conserved and medically-important nutrient sensing molecular pathways (insulin signaling and TOR) have on sexual attractiveness in a simple model system, Drosophila melanogaster. Our findings will help us to better understand the coevolution of individual condition and sexual attractiveness and may reveal molecular signatures of misregulated insulin/TOR pathways, which could be used as indicators in early diagnosis of many diseases, such as diabetes and heart disease.

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
5R01GM102279-03
Application #
8828241
Study Section
Genetic Variation and Evolution Study Section (GVE)
Program Officer
Sesma, Michael A
Project Start
2013-04-01
Project End
2017-03-31
Budget Start
2015-04-01
Budget End
2016-03-31
Support Year
3
Fiscal Year
2015
Total Cost
$290,601
Indirect Cost
$65,744
Name
University of Michigan Ann Arbor
Department
Physiology
Type
Schools of Medicine
DUNS #
073133571
City
Ann Arbor
State
MI
Country
United States
Zip Code
48109
Arbuthnott, Devin; Fedina, Tatyana Y; Pletcher, Scott D et al. (2017) Mate choice in fruit flies is rational and adaptive. Nat Commun 8:13953
Fedina, Tatyana Y; Arbuthnott, Devin; Rundle, Howard D et al. (2017) Tissue-specific insulin signaling mediates female sexual attractiveness. PLoS Genet 13:e1006935
Hoffman, Jessica M; Lyu, Yang; Pletcher, Scott D et al. (2017) Proteomics and metabolomics in ageing research: from biomarkers to systems biology. Essays Biochem 61:379-388
Harvanek, Zachary M; Lyu, Yang; Gendron, Christi M et al. (2017) Perceptive costs of reproduction drive ageing and physiology in male Drosophila. Nat Ecol Evol 1:152
Lee, Jung-Eun; Rayyan, Morsi; Liao, Allison et al. (2017) Acute Dietary Restriction Acts via TOR, PP2A, and Myc Signaling to Boost Innate Immunity in Drosophila. Cell Rep 20:479-490
Gendron, Christi M; Pletcher, Scott D (2017) MicroRNAs mir-184 and let-7 alter Drosophila metabolism and longevity. Aging Cell 16:1434-1438
Ro, Jennifer; Pak, Gloria; Malec, Paige A et al. (2016) Serotonin signaling mediates protein valuation and aging. Elife 5:
Harvanek, Zachary M; Mourão, Márcio A; Schnell, Santiago et al. (2016) A computational approach to studying ageing at the individual level. Proc Biol Sci 283:
Masel, Joanna; Promislow, Daniel E L (2016) Answering evolutionary questions: A guide for mechanistic biologists. Bioessays 38:704-11
Arbuthnott, D; Levin, T C; Promislow, D E L (2016) The impacts of Wolbachia and the microbiome on mate choice in Drosophila melanogaster. J Evol Biol 29:461-8

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