Scientist filling tubes, for article on reversible male contraception

Cornell researchers achieve first reversible male birth control in mice

For the first time, American researchers have shown that sperm production can be stopped and fully restarted in male mice — without hormones, without permanent effects, and without harming offspring. The breakthrough, published in April 2026 C.E. in the Proceedings of the National Academy of Sciences, brings a long-sought goal in reproductive medicine meaningfully closer to reality.

At a glance

  • Reversible male contraception: Cornell scientists used a small molecule called JQ1 to halt sperm production in male mice for three weeks, then stopped treatment — and within six weeks, normal sperm production returned completely.
  • Nonhormonal approach: Unlike most contraceptive research, this method targets meiosis directly in the testis, leaving libido and secondary sex characteristics entirely unaffected.
  • Healthy offspring: Mice that recovered fertility after treatment bred successfully, and their pups were also fertile — confirming no heritable damage from the intervention.

Why this matters

Right now, men have two main contraceptive options: condoms or vasectomy. Vasectomies are technically reversible through surgery, but the procedure is complex and success rates drop over time. No long-acting, fully reversible, nonhormonal option exists for men.

That gap carries real consequences. The global contraceptive burden falls disproportionately on women, many of whom face hormonal side effects ranging from mood changes to cardiovascular risk. Researchers have long hesitated to develop a male hormonal contraceptive for the same reasons. A safe, nonhormonal male option would shift that balance.

“We were really motivated to look for nonhormonal contraceptive targets in the testis,” said Paula Cohen, professor of genetics at Cornell’s College of Veterinary Medicine and director of the Cornell Reproductive Sciences Center. “Something that stops sperm production without affecting male libido and secondary sex characteristics.”

How the science works

Sperm production runs through three main stages. It begins with stem cells that replenish throughout a man’s life. Those cells then enter meiosis — the division process that halves the chromosome count to produce sex cells. After meiosis, a final stage called spermiogenesis shapes those cells into swimming sperm.

Cohen’s team targeted meiosis deliberately. Disrupting the stem cells would cause permanent infertility. Targeting spermiogenesis too late risked viable sperm surviving and escaping. The middle stage — meiosis, and specifically a phase called prophase 1 — turned out to be the right window.

The researchers used JQ1, a molecule originally developed to study cancer and inflammatory disease. It was never viable as a therapeutic drug because of neurological side effects, but it reliably disrupts prophase 1. That made it a precise research tool to prove the concept. After three weeks of JQ1 treatment, the mice produced no sperm at all. After treatment stopped, healthy sperm production resumed within six weeks. The mice then fathered fertile offspring with no abnormalities.

“Our study shows that mostly we recover normal meiosis and complete sperm function, and more importantly, that the offspring are completely normal,” Cohen said.

What comes next

JQ1 itself is not the end product — its neurological side effects rule that out. But it proved the principle. The team is now testing three new gene targets that, when disrupted, eliminate sperm production entirely in mice with no apparent health effects. The next step is confirming those targets can be switched on and off reversibly.

Cohen and her colleagues plan to launch a company within two years to advance the work toward human trials. If successful, the likely delivery format would be an injection every three months, or possibly a patch — designed to ensure consistent effectiveness. The Gates Foundation supported the research.

The study is co-first-authored by Stephanie Tanis and Leah Simon, both Ph.D. graduates from Cornell’s class of 2025, now postdoctoral researchers at the University of Colorado. Co-authors also include Jelena Lujic and Charles Danko from Cornell’s College of Veterinary Medicine.

It is worth being clear about where the science stands: this is a mouse study. The road from mice to a proven, approved human contraceptive is long, and many promising compounds fail to translate across species. Real-world efficacy, safety in humans, and delivery logistics all remain open questions.

Still, six years of careful work has produced something the field has never had before: a clear proof that meiosis in the testis can be targeted safely, stopped completely, and reversed without lasting harm. That is not a small thing. It is the foundation everything else gets built on.

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For more on this story, see: Cornell University News

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