#19,080
We've a fascinating, albeit somewhat controversial, study published last week in Cell which questions whether whether animal viruses must undergo some form of special adaptation before they can spill over into humans.
Obviously, we've looked at literally hundreds of spillovers (like Nipah, Ebola, H5Nx, Mpox, etc.) over the years, but the scientific consensus has been that these have been `flukes' - and that these viruses would have to further adapt to pose a serious public health threat.
As an example, we have a specific (and growing) watch list of `mammalian adaptations' (e.g. PB2 mutations like E627K, D701N, Q591K, and M631L and HA mutations like Q226L and E190D) that we look for in HPAI H5 (and other) influenza viruses.
Today's study suggests that - while these markers are still useful - many viruses with pandemic potential simply don't require prior-adaptation in order to jump species.
They just need opportunity.
As to the above-mentioned controversy, the authors state in a UCSD press release that they found:
No evidence that SARS-CoV-2 was shaped by selection in a laboratory or prolonged evolution in an intermediate host prior to its emergence. That absence of evidence is exactly what we would expect from a natural zoonotic event.
Since I don't have a dog in this fight, I'll simply acknowledge the elephant in the room and move on. The press release summarizes their main findings:
The prevailing model of zoonotic emergence has often assumed that viruses must first acquire adaptive mutations before they can sustain human-to-human spread. To test that assumption, the research team analyzed viral genomes from outbreaks caused by influenza A virus, Ebola virus, Marburg virus, mpox virus, SARS-CoV and SARS-CoV-2. They focused on the evolutionary period immediately preceding human outbreaks, where any substantial pre-spillover adaptation should leave a detectable imprint.
Across these diverse viruses, the investigators found a strikingly consistent pattern: selection pressures before zoonotic emergence were indistinguishable from those acting during routine circulation in animal reservoirs. In other words, there was no evolutionary signal suggesting that these viruses were being “pre-adapted” for humans prior to their outbreaks. Instead, measurable changes in selection typically appeared only after sustained transmission began in people.
“From a broad epidemiological standpoint, our findings challenge the idea that pandemic viruses are evolutionarily special before they reach humans,” Wertheim said. “Rather than requiring rare, finely tuned adaptations in animals, many viruses may already possess the basic capacity to infect and transmit between humans. What matters most is human exposure to a diverse array of animal viruses.”
I've posted the link and summary below, but there is a lot more to unpack, so you'll want to read the report in its entirety. I'll return with a bit more after the break.
Dynamics of natural selection preceding human viral epidemics and pandemics
Jennifer L. Havens 1 2 9, Sergei L. Kosakovsky Pond 3, Jordan D. Zehr 3 4, Jonathan E. Pekar 1 5 6, Edyth Parker 7, Michael Worobey 8, Kristian G. Andersen 7, Joel O. Wertheim 6S
https://doi.org/10.1016/j.cell.2026.02.006 Get rights and content
Under a Creative Commons license
HighlightsSummary
- Viral adaptation is not a necessary precursor to outbreaks of novel zoonotic viruses
- Selection signatures on SARS-CoV-2 were unchanged until its emergence in humans
- Laboratory and gain-of-function passage produce distinct evolutionary signatures
- 1977 influenza virus reemergence preceded by evolution consistent with laboratory passage
Using a phylogenetic framework to characterize natural selection, we investigate the hypothesis that zoonotic viruses require adaptation prior to zoonosis to sustain human-to-human transmission.
Examining the zoonotic emergence of Ebola virus, Marburg virus, mpox virus, influenza A virus, and SARS-CoV-2, we find no evidence of a change in selection intensity immediately prior to outbreaks in humans compared with typical selection within reservoir hosts.
We found a change in selection on SARS-CoV in an intermediate host.
We conclude that extensive pre-zoonotic adaptation is not necessary for human-to-human transmission of zoonotic viruses. In contrast, the reemergence of H1N1 influenza A virus in 1977 was preceded by a shift in selection intensity, consistent with the hypothesis of passage in a laboratory setting.
Holistic phylogenetic analysis of selection regimes can be used to detect evolutionary signals of host switching or laboratory passage, providing insight into the circumstances of past and future viral emergence.
(SNIP)
In this study, we have distinguished epidemics that are characterized by viruses that evolved primarily under a selection regime in the natural host reservoir prior to emergence from those that did not. Humans are constantly exposed to animal viruses.58,71 However, most of these exposures do not result in ongoing outbreaks with human-to-human transmission, due to low fitness of the virus or lack of sufficient transmission opportunities (such as in rural communities).72
In recent zoonotic epidemics with sustained human-to-human transmission, we found no detectable change in selection preceding the epidemics. Applying multi-region RELAX to the stem of novel viral outbreaks is a tool that we can apply to future outbreaks to rapidly assess the possibility of evolution in an intermediate host or a laboratory setting, compared with zoonosis directly from the natural host reservoir. Increased sampling of viruses in reservoir species will improve the power of approaches for investigating future zoonotic outbreaks.
While we comfort ourselves with the notion that we'd see distinct changes in the H5Nx virus that would telegraph when it was ready for prime time, today's study warns that such changes may not be necessary for the virus to jump to humans.
The authors wrote: `These findings challenge the model in which zoonotic viruses must progressively evolve the ability to sustain human-to-human transmission.'
In 2024, after nearly 30 years of continual circulation in Mexico, the LPAI H5N2 virus abruptly jumped to a 58-year-old immunocompromised patient - who had been bedridden for weeks - and had no obvious exposure risks.
The virus was a > 99% match with an avian LPAI H5N2 isolate from Texcoco, State of Mexico (2024), and showed no obvious signs of viral adaptation.
What series of events led to this first recorded human infection with LPAI H5N2 remains a mystery, but serological studies of poultry workers suggest that these types of infections probably happen more often than we know (see Taiwan: Three Poultry Workers Show H5N2 Antibodies).
While these spillovers have thus far failed to spread efficiently in humans, each spillover is another opportunity for the virus to better adapt to a human host.
Although we might see the next pandemic coming, our continued resistance to greatly increasing surveillance and testing of wildlife and livestock, and of humans that have routine exposure to those animals or their environments, makes any early warning far less likely.
