<div dir="ltr"><br><div class="gmail_extra"><br><div class="gmail_quote">On Fri, Aug 5, 2016 at 2:22 AM, Adrian Tymes <span dir="ltr"><<a href="mailto:atymes@gmail.com" target="_blank">atymes@gmail.com</a>></span> wrote:<br><blockquote class="gmail_quote" style="margin:0 0 0 .8ex;border-left:1px #ccc solid;padding-left:1ex"><div dir="ltr"><div><div><div>So let's take a diversion from the current threads.<br><br><a href="http://www.sciencemag.org/news/2016/08/new-theory-suggests-female-orgasms-are-evolutionary-leftover" target="_blank">http://www.sciencemag.org/<wbr>news/2016/08/new-theory-<wbr>suggests-female-orgasms-are-<wbr>evolutionary-leftover</a><br><br></div>If this theory is true, which of the following modifications might be more popular, and why? Assuming sufficiently advanced biotechnology, but these do not seem like they would require as radical a leap as some other technologies we have discussed.<br><br></div>1) Reverse evolution so that ovulation occurs upon orgasm. Celibate (or at least non-orgasming) females would be able to store their eggs longer (for career, et cetera), though they might take longer to mature sexually. On the flip side, deliberately getting pregnant would be easier since one could reliably induce ovulation without expensive medicines or procedures.<br><br></div>2) Modify the ovaries to be like the testes: constantly producing seed (egg cells, in their case). No more menopause.</div></blockquote><div><br></div><div>### There is a limited number of primordial ova in the ovary, and although the precise reason for this arrangement is not definitely known, the hypothesis that I favor goes as follows:</div><div><br></div><div>Mitochondrial DNA quality is crucial for the normal functioning of the organism. During cell division there is ample opportunity to accumulate mitochondrial mutations by random drift, and normal cellular metabolism also contributes to mtDNA mutations. Since you don't want to let your offspring inherit faulty mtDNA, the germ cell that contains it must be then appropriately protected, and in humans only the primordial ovum carries mtDNA. Primordial ova are very peculiar cells, with suppressed metabolism, non-dividing, large (makes random drift in mtDNA less problematic), which appears to be ideal kind of cell to keep mtDNA safe. But mtDNA still undergoes decay, which is why the average quality of ova goes down from age 25 onward, hundreds of thousands of them are automatically culled at mitochondrial metabolic checkpoints, until at age 40 most women become infertile from an exhaustion of ova.</div><div><br></div><div>Sperms to not carry mtDNA, and therefore the constraints that apply to ova are not relevant to them.</div><div><br></div><div>Changing ova production to match sperm in amount and duration would require some quite advanced biological tinkering.</div><div><br></div><div>Rafał</div><div><br></div><div>Rafał</div></div>
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