'Gain of function' research can create experimental viruses. In light of COVID, it should be more strictly regulated – or banned

The United Nations Environment Programme recently published a scientific review^[1] that looks at environmental threats and risks in light of the COVID pandemic. It analyses links between human infectious diseases and nature and what we know about how diseases (zoonoses) can transfer from animals to humans.

The report (which I wrote) argues laboratory procedures (including “gain of function” research) should be recognised as one potential driver of zoonotic “spillover”.

The term “gain of function” applies to the functional consequences of changes in the genetic makeup of an organism, including viruses. Such changes can be harmless, or even beneficial. They can occur naturally, when organisms mutate and evolve.

But experiments to deliberately induce mutations are increasingly done in laboratories. In that context, gain of function generally refers to attempts to confer greater transmission and/or virulence to a virus.

Supporters of such research argue it promises to help us be better prepared for pandemics. They acknowledge^[2] risks, but argue these can be managed by the use of highly regulated^[3] secure laboratories. Others maintain that the potential risks are simply too high and this type of research should be banned^[4].

Read more: Why gain-of-function research matters^[5]

How DNA discoveries led to ‘gain of function’ research

During the second world war, DNA (and later RNA) was identified^[6] as the key genetic molecule. DNA’s (and RNA’s) structure provides unique “instructions” for every living organism.

Within just three decades “recombinant^[7]” technology made it possible to splice together genetic material from different species. Today, this can be done with consummate ease.

Numerous benefits followed, such as the insertion of insulin-producing genes into bacteria. This enabled cheaper, large-scale production^[8] of this hormone, essential to treat type I diabetes.

A 2019 report^[9] valued the market in therapeutics, mostly arising through recombinant genetic technologies, at more than US$315 billion (A$490 billion). The use of crops genetically engineered to resist disease^[10] is also increasing.

However, this type of research also sparked debate and concern.

A key figure in this emerging technology was Paul Berg, a biochemist who shared the 1980 Nobel Prize. Berg’s early work focused on modifying the SV-40 virus, known to be involved in tumour growth^[11]. Berg abandoned an experiment, inserting SV-40 into a bacterium, for fear, expressed by “many colleagues^[12]” that the newly created organism might infect humans, causing cancer.

For the next few decades, scientists navigated the complex ethics and developing technology around gene splicing, under increasingly secure conditions^[13] to limit foreseeable biohazard risks.

Bird flu

Then, in 2011, researchers performed experiments with a bird flu virus called H5N1. The virus killed an alarming percentage of humans diagnosed^[14] with it. Its saving grace was that it had very poor human-to-human transmission.

Controversy^[15] arose when two teams of researchers explored and found ways to make H5N1 transmissible between mammals. After first genetically modifying H5N1 researchers performing “serial passage” experiments in a mammalian model (ferrets) to see if they could further adapt it for mammalian to transmission. They succeeded.

Although it wasn’t clear the virus would be as deadly in humans, critics worried this new strain might escape (even from highly secure labs) and cause millions of deaths.

These concerns led US authorities to delay the studies’ full publication and to later restrict funding guidelines^[16]. This was intended to reduce genetic experiments perceived as risky.

References

1. ^{^} scientific review (wedocs.unep.org)
2. ^{^} acknowledge (www.technologyreview.com)
3. ^{^} highly regulated (www.nature.com)
4. ^{^} banned (www.cidrap.umn.edu)
5. ^{^} Why gain-of-function research matters (theconversation.com)
6. ^{^} identified (journals.plos.org)
7. ^{^} recombinant (www.ncbi.nlm.nih.gov)
8. ^{^} large-scale production (doi.org)
9. ^{^} 2019 report (www.grandviewresearch.com)
10. ^{^} resist disease (doi.org)
11. ^{^} tumour growth (doi.org)
12. ^{^} many colleagues (www.nobelprize.org)
13. ^{^} secure conditions (absa.org)
14. ^{^} diagnosed (doi.org)
15. ^{^} Controversy (journals.asm.org)
16. ^{^} restrict funding guidelines (doi.org)
17. ^{^} dual use (doi.org)
18. ^{^} misused for harm (www.who.int)
19. ^{^} a more careful stance (doi.org)
20. ^{^} Cambridge Working Group declaration (www.cambridgeworkinggroup.org)
21. ^{^} Working with dangerous viruses sounds like trouble – but here's what scientists learn from studying pathogens in secure labs (theconversation.com)
22. ^{^} true origin (theconversation.com)
23. ^{^} framework (www.who.int)
24. ^{^} concerns (www.mja.com.au)
25. ^{^} review (www.nhmrc.gov.au)
26. ^{^} work (doi.org)
27. ^{^} potential risks (theintercept.com)
28. ^{^} The COVID lab leak theory is dead. Here's how we know the virus came from a Wuhan market (theconversation.com)