Intergenerational Influence of Paternal Obesity on Metabolic and Reproductive Health Parameters of the Offspring: Male-Preferential Impact and Involvement of Kiss1-Mediated Pathways.
Sanchez-Garrido. Miguel Angel MA; Ruiz-Pino. Francisco F; Velasco. Inmaculada I; Barroso. Alexia A; Fernandois. Daniela D; Heras. Violeta V; Manfredi-Lozano. Maria M; Vazquez. Maria Jesus MJ; Castellano. Juan Manuel JM; Roa. Juan J; Pinilla. Leonor L; Tena-Sempere. Manuel M
Key Findings
- Male offspring of obese fathers gain more weight and have higher leptin on a high‑fat diet than those of lean fathers.
- Paternal obesity lowers baseline LH levels and worsens the drop in testosterone and related gene expression in male offspring on a high‑fat diet.
- Both male and female offspring from obese fathers show reduced LH responses to central kisspeptin‑10 administration, with a stronger effect in males.
Practical Outcomes
- For biohackers interested in using kisspeptin‑10 to boost reproductive hormones, the study suggests that metabolic health (especially paternal obesity and a high‑fat diet) can blunt its effectiveness, particularly in men. Optimizing diet and body composition may be a prerequisite for getting reliable kisspeptin responses. The findings do not provide new dosing guidelines but highlight the importance of addressing underlying metabolic factors before relying on kisspeptin‑based protocols.
Summary
The study shows that when fathers are obese, their male offspring who later eat a high‑fat diet gain more weight, have higher leptin, and show weaker hormone (LH) responses to kisspeptin‑10, which could lower testosterone. Female offspring are less affected metabolically, but both sexes have a blunted LH response to kisspeptin. In short, paternal obesity makes the male offspring’s metabolism and reproductive hormone system more vulnerable, and it also dampens how well kisspeptin works.
Abstract
Obesity and its comorbidities are reaching epidemic proportions worldwide. Maternal obesity is known to predispose the offspring to metabolic disorders, independently of genetic inheritance. This intergenerational transmission has also been suggested for paternal obesity, with a potential negative impact on the metabolic and, eventually, reproductive health of the offspring, likely via epigenetic changes in spermatozoa. However, the neuroendocrine component of such phenomenon and whether paternal obesity sensitizes the offspring to the disturbances induced by high-fat diet (HFD) remain poorly defined. We report in this work the metabolic and reproductive impact of HFD in the offspring from obese fathers, with attention to potential sex differences and alterations of hypothalamic Kiss1 system. Lean and obese male rats were mated with lean virgin female rats; male and female offspring were fed HFD from weaning onward and analyzed at adulthood. The increases in body weight and leptin levels, but not glucose intolerance, induced by HFD were significantly augmented in the male, but not female, offspring from obese fathers. Paternal obesity caused a decrease in luteinizing hormone (LH) levels and exacerbated the drop in circulating testosterone and gene expression of its key biosynthetic enzymes caused by HFD in the male offspring. LH responses to central kisspeptin-10 administration were also suppressed in HFD males from obese fathers. In contrast, paternal obesity did not significantly alter gonadotropin levels in the female offspring fed HFD, although these females displayed reduced LH responses to kisspeptin-10. Our findings suggest that HFD-induced metabolic and reproductive disturbances are exacerbated by paternal obesity preferentially in males, whereas kisspeptin effects are affected in both sexes.
Study Information
pubmed
2018
2018-02-01T00:00:00.000Z
10.1210/en.2017-00705
47
48