We Already Legalized "Designer Babies" Decades Ago — We Just Didn't Call Them That

In the immediate term — the next six months — the most predictable development is the paper's journey through formal peer review and eventual publication in a top journal. Egli's preprint was posted to bioRxiv on June 1, 2026, without yet clearing peer review. Once it publishes in Nature or Science, public conversation will scale dramatically relative to what we've seen so far. In the U.S., FDA regulations currently prohibit clinical trials of human germline editing through a rider on the annual Consolidated Appropriations Act. Critically, this is not permanent law — it gets renewed annually and could theoretically be reversed or permanently codified in either direction. I give roughly 70% odds that formal publication of Egli's results triggers congressional hearings, with advocates on both sides pushing hard for different legislative outcomes. This will be the most important near-term regulatory moment for this technology in the United States.

In the UK, the Human Fertilisation and Embryology Authority operates independently of the Oviedo Convention, which the UK never signed. Depending on how HFEA interprets this research, a scenario in which the UK becomes the first jurisdiction to authorize tightly controlled germline research trials — not clinical application, but supervised laboratory research — is not impossible. That would represent a significant geopolitical moment and would put enormous pressure on other European regulators to define their positions more precisely than they have so far. Europe's internal division between Oviedo Convention signatories and non-signatories means there is no unified European stance, and this vacuum creates room for regulatory divergence that commercial interests will be watching closely.

One additional short-term variable deserves attention: China. After He Jiankui, China toughened criminal penalties for germline editing in 2019. But it simultaneously pursues the world's most aggressive program of somatic gene therapy clinical trials. As of 2026, China has active CRISPR-based trials for blood disorders, cancer, and other conditions numbering in the dozens. The technical infrastructure required for germline editing isn't far removed from this somatic work — it's adjacent, not distant. I estimate roughly a 40% probability that informal germline research is already underway below the threshold of regulatory visibility. He Jiankui himself was released from prison in 2024 after serving his three-year sentence, and where his expertise went is not publicly documented. That is not a trivial concern.

In the medium term — six months to two years out — the commercial landscape will begin to reshape significantly. The global gene therapy market was estimated at approximately $13 billion in 2025, projected to reach $26 billion by 2028. Egli's results function as a proof of concept that will attract substantial venture capital interest in germline editing pipelines. I expect at least three to five additional biotech startups to quietly begin constructing germline editing programs alongside existing players. The pivotal actors to watch are Beam Therapeutics — which holds key base editing patents and whose roughly $4.5 billion market cap could double or triple if a clinical pathway opens — and the Broad Institute group around David Liu, the scientist who invented base editing technology itself. Liu has been publicly responsible about the applications of his invention; how he positions himself publicly as commercial pressure mounts will be a critical signal for the whole field.

Equally important in the medium term is the question of international regulatory coordination — or the absence of it. Right now, no internationally binding agreement on human germline editing exists. WHO published a genome editing governance framework in 2021, but it is purely advisory. I estimate roughly 55% probability that, by 2027, a UN or WHO-level process to negotiate a binding convention will have formally begun. But even if negotiations start promptly, a treaty with real enforcement mechanisms will take a minimum of five additional years to finalize and ratify. That gap — from research milestone to enforceable law — is where regulatory arbitrage will flourish. Clinics will establish themselves in jurisdictions with limited oversight, offering high-cost services to the global affluent. The stem cell tourism of the 2000s is the relevant precedent, and embryo editing tourism is more commercially attractive by orders of magnitude.

Looking further ahead, the two-to-five year horizon presents three distinct scenarios. The optimistic scenario, which I assign roughly 20% probability, involves the international community moving with unusual speed: a governance framework is established that permits embryo editing strictly for severe single-gene disorders under rigorous oversight, with independent verification and international data sharing required as conditions of authorization. Under this scenario, the first authorized clinical research programs for conditions like sickle cell disease and cystic fibrosis could begin around 2029 or 2030. The public health impact would be profound — sickle cell disease affects approximately 300,000 newborns annually, disproportionately in sub-Saharan Africa, where it remains a leading cause of under-five mortality. The reason I assign only 20% to this outcome is not technical infeasibility but historical reality: international consensus on topics intersecting deeply held religious values and enormous commercial interests has consistently proven extraordinarily slow. Nuclear nonproliferation, climate agreements, pandemic preparedness — the track record is not encouraging.

The baseline scenario, at roughly 55% probability, is one of suspended animation: major regulatory jurisdictions maintain current prohibitions on clinical germline editing while permitting continued laboratory research, pushing clinical questions past 2030. During this window, data accumulates from animal studies — particularly non-human primate models — and scientific understanding of base editing safety, mosaicism, and long-term developmental effects gradually improves. The problem is that technology keeps advancing and commercial pressure keeps building during this same window, steadily widening the gap between technical possibility and legal permission. I estimate roughly 35% probability that by 2028 at least one unauthorized germline editing birth will be reported from a low-oversight jurisdiction — a second He Jiankui moment, but with technology that is demonstrably more refined, making continued prohibition harder to defend on purely technical-safety grounds than it was in 2018.

The pessimistic scenario, at roughly 25% probability, is the one that concerns me most: unregulated commercialization advances faster than law, and a de facto market for premium embryo editing services establishes itself in regulatory grey zones. Initial pricing in the $500,000 to $1 million range places this within reach of the top one to five percent of global income earners — the same demographic that purchases Manhattan real estate as a portfolio hedge. As technical costs decline over five to seven years, the accessible population widens, but regulatory and equity frameworks still don't exist. The most sobering feature of this scenario is intergenerational compounding. A family that uses this technology in 2028 transmits optimized genetic sequences to every subsequent generation, automatically, without further cost or intervention. Against current global wealth distribution — where the top 10% control roughly 76% of all assets — adding a biological multiplier to that concentration produces a form of stratification that no redistribution mechanism in our current political toolkit can address.

I should be honest about the ways this analysis could be wrong. Mosaicism may turn out to be a more fundamental technical barrier than current optimism implies, delaying safe clinical application by a decade or more beyond what today's efficiency numbers suggest. In vitro results do not automatically predict what happens during actual embryonic development after implantation, and the gap between laboratory efficiency and developmental biology has surprised researchers repeatedly in the history of genetics. Public moral opposition could prove more durable and politically consequential than technological optimism typically accounts for — the European response to GMOs, sustained and politically effective despite scientific consensus on safety, is the most relevant precedent. Populations can and do maintain categorical prohibitions on technologies associated with "playing God," and that moral intuition should not be easily dismissed as irrational.

The most practical thing I can offer: watch the regulatory calendars. Watch what the UK's HFEA decides in its response to Egli's results. Watch whether the U.S. Congress allows the germline editing appropriations rider to lapse or makes it permanent law. Watch where Beam Therapeutics and the Broad Institute publicly position themselves on clinical application, because their choices will signal which direction commercial momentum is headed. If you have any capacity to participate in public bioethics consultations — national ethics boards, academic forums, policy comment periods — use it. This is not a decision that should be made by scientists, investors, and regulators in isolation from the people whose children will live in the world those decisions create. The question of whether genetic advantage becomes the next frontier of inherited privilege is one the entire public has a stake in answering, and it is being decided right now.