Friday, June 05, 2026

FluView Week #20: EOY Review of Increased Detection of Oseltamivir Resistant H1N1 Viruses


Abrupt rise in Oseltamivir resistance in Catalonia, Spain - fall 2025

#19,189

For the past 3 years we've been following sporadic reports of `reduced susceptibility' of the seasonal H1N1 flu virus to the antiviral drug oseltamivir (aka `Tamiflu') around the globe (see EID Journal: Multicountry Spread of Influenza A(H1N1)pdm09 Viruses with Reduced Oseltamivir Inhibition, May 2023–February 2024).

While concerning, these reports indicated reduced inhibition - not complete failure - and its incidence has been modest; typically in the low single digits.   
The main culprit in all of this has been an increase in the S247N mutation (often combined with I223V), which can reduce the effectiveness of oseltamivir 7 to 16 fold. 

Less common, but far more impactful, is the H275Y mutation, which can effectively render oseltamivir useless. This was the cause of the `Tamiflu failure' of 2008, which temporarily forced the CDC to change their flu treatment guidelines.

Luckily, the arrival of a new, and still susceptible pandemic H1N1 virus in 2009 granted oseltamivir an unexpected reprieve, but since then we've kept a close eye out for any genetic changes that could affect its effectiveness. 

Last summer, in Virus Research: A 15-year Study of Neuraminidase Mutations and the Increasing of S247N Mutation in Spain, we looked at a study that found a sharp increase in detections of the S247N mutation beginning in 2024. 

Highlights

• In a landscape of a very narrow arsenal of influenza antivirals, resistance mutations are a significant threat.

• Resistance mutations were present in 0.5-5% in A and B influenza viruses during the last 15 years.

• However, S247N resistance mutation in the NA gene sharply increased during 2023-2024 season.

• While this mutation does not confer strong resistance by itself, their fixation could increase the risk of resistance in the future if other resistance mutations appears or get fixed together with it
Over the 2025-2026 flu season we've continued to see scattered reports of resistance, including Taiwan's CDC reported that 6.5% of the H1N1 viruses characterized in 2025 showed signs of oseltamivir resistance, and China: National Influenza Center Reporting Increased Oseltamivir Resistance in Seasonal H1N1

As for detections in the United States, as we saw last February, over the entire 2024-2025 flu season - out of 1697 H1N1 viruses tested - only one carried the NA-I223V and NA-S247N amino acid substitutions.

And reassuringly, during the first 13 weeks of the 2025-2026 flu season (Oct - Dec) the CDC reported zero elevated resistance among the first 193 H1N1 viruses tested (see screenshot from FluView Wk 53).  


But by the end of February, 2026 (FluView Week 7), things had begun to change. Based now on 517 H1N1 isolates tested since October 2026 - the CDC reported 10 viruses with reduced susceptibility and 4 with highly reduced inhibition.

Four A(H1N1)pdm09 viruses had NA-H275Y amino acid substitution conferring highly reduced inhibition by oseltamivir and peramivir. Ten A(H1N1)pdm09 viruses had amino acid substitutions NA-I223V and NA-S247N and showed reduced inhibition by oseltamivir. Two B viruses had amino acid substitution NA- M464T and showed reduced inhibition by peramivir.
Last Friday the CDC published their last full FluView report of the 2025-2026 flu season (week 20), which contained the following brief update on oseltamivir resistant viruses. 



Nine A(H1N1)pdm09 viruses had NA-H275Y amino acid substitution conferring highly reduced inhibition by oseltamivir and peramivir. Nineteen A(H1N1)pdm09 viruses had amino acid substitutions NA-I223V and NA-S247N and showed reduced inhibition by oseltamivir. One A(H1N1)pdm09 virus had amino acid substitutions NA-I223T and NA-S247N and showed reduced inhibition by oseltamivir. Two A(H3N2) viruses had amino acid substitution NA-E119V conferring highly reduced inhibition by oseltamivir. Three B viruses had amino acid substitution NA-M464T and showed reduced inhibition by peramivir.


While the number of S247N+I223V mutations remains low (2.1%), this is more than a 35-fold increase over the previous year, making this a trend well worth following. 

The incidence of the far more impactful H275Y mutation (1%) remains about average, but there are concerns that the stacking of H275Y with either I223V or S247N could greatly enhance its impact.

None of this is to suggest we are on the verge of another antiviral crisis, only that we continue to see some concerning trends. And given the gaps in global influenza surveillance and reporting, we are only seeing part of the picture.

As we are so frequently reminded - evolution never stops - and while our current antiviral armamentarium remains effective against seasonal H1N1, the events of 2008 reminds us how quickly that can change. 

Stay tuned.

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Thursday, June 04, 2026

USDA: USDA Confirms Presence of New World Screwworm in the United States

 

#19,188

The New World Screwworm (NWS aka Cochliomyia hominivorax) - which was eliminated in the United States during the 1960s - is a flesh-eating parasitic fly that lays its eggs in the open wounds of warm-blooded animals (often cattle and deer, but occasionally humans).

Unlike most fly maggots, which feed on dead tissue, NWS larva consume and burrow into live tissue, causing substantial morbidity and mortality. (See ASM 2025 Review New World Screwworm: Rise, Fall and Resurgence).

During the 1980s, eradication efforts - primarily utilizing the Sterile Insect Technique (SIT) - expanded NWS elimination southward through Mexico and Central America, to the Darien Gap in  Panama where for many years (starting in 1996) the line was held. 

But in 2023, the number of screwworm detections in Panama surged from a few dozen to thousands, and the infestation began moving northward again. While likely due to a myriad of reasons - including climate change and human migration - supply chain issues during the COVID pandemic is often cited as a factor. 

Since then, the NWS has been moving north steadily, and has been reported getting closer to the U.S./Mexico border in recent months. In August of last year, the HHS reported a Singular Traveler-Associated New World Screwworm Case

The USDA has produced its own projections of the economic impact of NWS (in 2024), which finds it could cost Texas farmers nearly 2 billion dollars a year.



Not unexpectedly, last night the USDA announced the first detection of NWS on a farm in Southern Texas. While this is not a big public health concern, should it spread widely, it could prove quite costly to the cattle industry. 
Last night's announcement focuses primarily on reassuring the public (about food safety, and that authorities are responding aggressively). While serious, for now this remains a single detected incursionnot evidence of established transmission within the United States.   
First the announcement from the USDA (h/t to Sharon Sanders on FT for the head's up), after which I'll have a bit more. 

USDA Confirms Presence of New World Screwworm in the United States

Contact: aphispress@usda.gov

Animal Health Officials Working Quickly to Protect U.S. Livestock and Wildlife

WASHINGTON, DC, JUNE 03, 2026 – The U.S. Department of Agriculture’s (USDA) Animal and Plant Health Inspection Service (APHIS) confirmed the detection of a New World screwworm (NWS) in a bovine in Zavala County, Texas. NWS is a serious pest that affects livestock, pets, wildlife, and less commonly, people and birds. NWS larvae (maggots) burrow into the flesh of living animals, causing serious damage to livestock and economic losses.

The affected animal is a 3-week-old calf and larvae were identified in its umbilical area. To date, there have been no further detections.

“All models showed New World Screwworm entering the country in 2025; however, thanks to the hard work across the entire Trump administration and our industry, state, and local partners, we were able to buy time for this moment. Protecting our livestock industry is a national security issue of the utmost importance, and USDA is wasting no time in taking action,” said Dudley Hoskins, Under Secretary for Marketing and Regulatory Programs. “USDA invested heavily in the tools needed to eliminate NWS ever since cases started increasing in Central America and Mexico. The United States has defeated this pest before, and we will do it again.”

USDA and Texas officials are taking immediate action to contain and eradicate NWS from the United States, following the strategies and actions outlined in the NWS Response Playbook. This includes:
  • Forming a unified Incident Command Team with the Texas Animal Health Commission and deploying response personnel to the area;
  • Establishing a 20 km infested zone around the detection and implementing quarantines, movement controls, and surveillance in this area;
  • Expediting targeted release of sterile NWS flies by immediately deploying ground release chambers in the area, in addition to the 4 million sterile flies per week already being released aerially in the area;
  • Increasing trapping for NWS flies along the border and just outside of the dispersal area;
  • Implementing NWS surveillance and management strategies in wildlife; and
  • Conducting targeted outreach in the local area.
Additionally, USDA’s National Veterinary Stockpile stands ready to assist, and will provide resources including treatments, equipment, and logistics support the response as needed.

USDA will continue to work with state departments of agriculture, animal health officials, industry, and producers to mitigate economic impacts of restrictions as much as possible, including negotiating with our trading partners to regionalize any trade restrictions on live animals, limiting them to defined geographic areas.

NWS maggots can infest livestock and other warm-blooded animals, including in rare cases people. They most often enter an animal through an open wound and feed on the animal’s living flesh.

USDA urges residents in the area to check their pets and livestock for signs of NWS. Look for draining or enlarging wounds and signs of discomfort. Also look for screwworm larvae (maggots) and eggs in or around body openings, such as the nose, ears, and genitalia or the navel of newborn animals. If you suspect your animal is infected with screwworm, contact your state animal health official or USDA area veterinarian in charge immediately.

While not common in people, if you notice a suspicious lesion on your body or suspect you may have contracted screwworm, seek immediate medical attention.

The U.S. food supply is safe. Screwworms do not infest meat, fruits, vegetables, or other food sources. USDA’s Food Safety and Inspection Service (FSIS) ensures that the nation’s commercial supply of meat, poultry, and egg products is safe and properly labeled. Under the Federal Meat Inspection Act (FMIA), FSIS inspection personnel must inspect all eligible animal species unless they are exempt or covered by a state inspection program.

Any evidence of screwworm infestation in an animal would be identified during these inspections, and any contaminated product from an affected animal would not be allowed to enter the food supply.

For more than a year, USDA has led a unified response to NWS. As the lead coordinating agency, USDA has deployed advanced surveillance systems and supported robust cross-border response efforts in Mexico and Central America to combat the pest and push NWS away from the United States. These efforts have bought time for USDA to increase domestic preparedness efforts.

Learn more about New World screwworm at Screwworm.gov.


All this comes at a particularly bad time, since U.S. cattle inventories are already at their lowest level in decades (due to prolonged droughts and high feed costs), and beef prices are at record highs. 

 As we've seen previously, the introduction (or reintroduction) of agricultural and human diseases can be difficult to contain. A few examples include:

The good news is the USDA has known this day was coming, and has been actively preparing for it. Last April, the USDA released an Updated New World Screwworm Response Playbook, and in January announced the  Completion of Sterile Fly Dispersal Facility in Texas

With a little luck, this breach can be contained.  

But as long as the NWS continues to circulate in Mexico, future incursions are all but inevitable. And with all such border interdictions, the defender must succeed 100% time, while the invader only has to succeed once. 
  
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Wednesday, June 03, 2026

Preprint: Increased burden of influenza A/H1N1pdm09 in older adults following the COVID-19 pandemic


#19,187

If there is one constant with influenza A viruses, it is that they are constantly changing; meaning that things that we may have assumed to be true for years or even decades can abruptly change.  

One such `truism' has been that H1N1 viruses pose more of a risk to younger individuals - those born after the 1957 H2N2 pandemic emerged - than to the elderly (see PLoS Path.: Childhood Immune Imprinting to Influenza A).

While older individuals weren't immune to H1N1, they have tended to be less susceptible to infection - and typically saw milder disease - than from the H3N2 subtype.

At least - according to a preprint published last week - until 2022, when a new clade of H1N1 emerged (6B.1A.5a.2a) after the COVID-19 induced lull, which appears to have become more impactful on the elderly. 

Although it was overshadowed by the outbreaks of early May (hantavirus & Ebola), the JID reported a similar finding (see Effects of Age and Birth Cohort on Influenza A Virus Subtype-Specific Hospitalization Rates, United States, 2010–2025) in late April.
 
Assuming these reports are correct, the notion that the elderly might enjoy a bit of a respite during H1N1 centric flu seasons may no longer be true, and that could substantially increase the burden on healthcare facilities. 

An additional caveat: it has not been established whether (or how strongly) this pattern will persist as H1N1 continues to evolve.  Clade 5a.2a has already been largely replaced by newer subclades (see week 20 FluView), so ongoing surveillance and analysis is needed. 

 
First, the link and some excerpts from the preprint, but the full report is very much worth reading.

Increased burden of influenza A/H1N1pdm09 in older adults following the COVID-19 pandemic
Simon P. J. de Jong, Colin A. Russell
doi: https://doi.org/10.64898/2026.05.20.26353664
This article is a preprint and has not been peer-reviewed

Preview PDF

Abstract

Of the two influenza A virus (IAV) subtypes circulating endemically in humans, A/H3N2 and A/H1N1pdm09, A/H3N2 has historically been the dominant driver of disease burden in older adults. Based on an analysis of publicly available global surveillance data from 2015 to 2025 (>300,000 subtyped, age-stratified infections), we report a substantially increased contribution of A/H1N1pdm09 to influenza morbidity in older adults since approximately 2022.

Birth cohort-stratified analyses suggest elevated A/H1N1pdm09 burden among individuals born before 1955-1959, consistent with erosion of pre-existing immunity originally generated by exposure to historical A/H1N1 strains. Pooled estimates across datasets and analytical approaches indicate the increase in A/H1N1pdm09 burden rises with earlier birth year, ranging from 1.22-fold (95% CI 1.08-1.37) for the 1955-1959 birth cohort to 3.10-fold (95% CI 2.58-3.72) for the 1930-1934 cohort. These findings point to a substantial rise in the overall influenza burden among the most vulnerable age groups, with implications for vaccine policy, clinical management, and public health planning.

Main text

Older adults are at markedly elevated risk of severe outcomes from influenza. Of the two influenza A virus (IAV) subtypes currently circulating in humans, A/H3N2 and A/H1N1pdm09, A/H3N2 has historically disproportionately contributed to influenza burden in older adults1,2. However, emerging evidence suggests possible shifts in this epidemiological landscape. A recent US-based study reported increasing contributions of A/H1N1pdm09 virus infections to influenza hospitalizations among older adults since the COVID-19 pandemic3.

        (SNIP)


The apparent increases in A/H1N1pdm09 risk are greatest in the earliest birth cohorts (Fig. 2). This could have substantial clinical and public health implications, as risk of severe influenza disease and mortality increases strongly with age5,6. As such, our results have implications for healthcare capacity planning, with likely substantially elevated acute and post-acute healthcare demand due to influenza compared to a counterfactual in which no immune erosion had occurred. The severity of the 2024/2025 US influenza season potentially reflects the erosion of protection in early birth cohorts3, with adults aged 75 and over experiencing the highest rates of A/H1N1pdm09-associated hospitalization since the 2009 pandemic16.

Vaccines have demonstrated effectiveness against A/H1N1pdm09 among adults aged 65 and over in the post-pandemic period17,18, but new targeted analyses in the earliest birth cohorts, for which estimated increase in burden is greatest (Fig. 2), would be valuable. A potential concern is that individuals whose immunity was shaped predominantly by early-life responses to historical A/H1N1 epitopes may, through repeated boosting of those same responses, lack immunity to epitopes on strains circulating since 2022, leaving them with little cross-reactive protection to recall upon vaccination or infection. These uncertainties notwithstanding, the elevated A/H1N1pdm09 risk suggested here further strengthens the case for vaccination in these birth cohorts and has implications for vaccination strategies, including the value and cost-effectiveness of enhanced formulations which have demonstrated superior immunogenicity and effectiveness in older adults19.
The US and Brazil hospitalization data indicate increased burden of severe disease due to A/H1N1pdm09, but whether this is due to changes in infection risk and/or changes in clinical severity warrants further investigation, particularly given that A/H1N1pdm09 was associated with relatively severe outcomes among hospitalized adults before the COVID-19 pandemic20,21.
Our analyses rely on observational data and are susceptible to reporting biases; however, consistency across four surveillance systems with distinct ascertainment mechanisms and varying analysis methods makes a surveillance artifact implausible. Replication with additional age- and subtype-resolved surveillance data would further substantiate our findings.
Together, our results indicate that the earliest birth cohorts, who are the most clinically vulnerable and have historically been considered relatively protected from influenza A/H1N1pdm09, likely now face substantially elevated risk from these viruses.
This carries potential implications for vaccine policy and healthcare capacity planning. Ensuring that surveillance infrastructure captures age- and subtype-resolved influenza data globally will be essential for tracking this shift and quantifying its consequences for the populations most at risk for severe influenza.
        (Continue . . . )

We tend to think that next year's seasonal flu will be pretty much like last year's, and the year before.  But even non-pandemic flu viruses can throw us curves. 
All reasons why we should give seasonal flu the respect it deserves. 
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Tuesday, June 02, 2026

CMAJ: Acetaminophen in pregnancy

Photo Credit – Wikipedia

#19,186

Last September, following a White House announcement suggesting a link between acetaminophen use during pregnancy and rising rates of autism, we looked at a statement from the World Health Organization and other medical stakeholders which pushed back on the theory. 

While no drug can claim to be 100% safe in 100% of the people that take it, these OTC pain/fever relievers have long been considered the safest option for both the mother and unborn child.

We've looked at potential drivers of increased autism often over the years, and after genetics, environmental exposures - and increased recognition of those on the spectrum - fevers during pregnancy are frequently cited (see Molecular Psy.: Increased Autism Risk Linked To Prenatal Fever).

While a few studies have claimed a statistical link between acetaminophen use during pregnancy and autism (Link), none have found a causal link, and a large 2024 study found `Acetaminophen use during pregnancy was not associated with children’s risk of autism, ADHD, or intellectual disability in sibling control analysis.'

The concern is: disparaging the only `presumed safe' option to reduce maternal fevers could actually end up increasing the incidence of autism, instead of decreasing it.

We revisited this story last January in The Lancet: Prenatal Paracetamol Exposure and Child Neurodevelopment: A Systematic Review and Meta-Analysis, which incorporated 43 studies (17 of which were combined in the meta-analysis), which reported:

Current evidence does not indicate a clinically important increase in the likelihood of autism spectrum disorder, ADHD, or intellectual disability in children of pregnant individuals who use paracetamol as directed, supporting existing recommendations on its safety.
Additional research is still needed to better understand heavy or prolonged usage, but these findings should be reassuring to anyone who chooses to use these drugs during pregnancy.

Under Implications of all the available evidence, the authors wrote:

Taken together with large-scale sibling-controlled studies from Sweden and Japan published in 2024 and 2025, our findings support the safety of paracetamol when used appropriately during pregnancy. They reinforce the guidance of major professional and regulatory bodies, including the American College of Obstetricians and Gynecologists, the Royal College of Obstetricians and Gynaecologists, and the European Medicines Agency, which continue to recommend paracetamol as the first-line analgesic and antipyretic in pregnancy.
Avoiding paracetamol based on inconclusive or biased evidence might increase the risk of maternal fever or untreated pain, both of which can harm pregnancy outcomes. Future research should focus on improving exposure measurement, standardising outcome definitions, and integrating mechanistic and family-based designs to clarify any residual uncertainties.

Admittedly, not a rock solid 100% guarantee of absolute safety; but in life, precious little is. 

Weighing in on all of this, yesterday the CMAJ published a brief review on the use of acetaminophen in pregnancy, and they too find that `Current evidence does not indicate a causal link between acetaminophen use in pregnancy and adverse infant outcomes.'

For those looking for a bit more reassurance, I've posted their report below. 

Acetaminophen in pregnancy
Jonathan S. Zipursky Rachela Smith and Tali Bogler CMAJ
June 01, 2026
DOI: https://doi.org/10.1503/cmaj.260138
PDF

Acetaminophen is the preferred analgesic and antipyretic agent for pregnant people

More than half of pregnant people use acetaminophen, most commonly for pain.1 Compared with alternatives, acetaminophen is the best studied analgesic and antipyretic in pregnancy and has the most reassuring maternal and fetal safety profiles. Major regulatory and obstetrical organizations support judicious use of acetaminophen as the first-line treatment for fever and pain in pregnancy.2

Studies on the risks of neurodevelopmental disorders related to acetaminophen use in pregnancy have not established causation

Some systematic reviews suggest small associations between prenatal acetaminophen use and autism spectrum disorder and attention-deficit/hyperactivity disorder. However, studies that rigorously control for potential confounders or emphasize sibling-controlled designs have typically found weaker or null associations.3,4 This suggests that unmeasured confounders (e.g., genetic and environmental factors) largely explain the associations with neurodevelopmental disorders.5 Randomized controlled trials have not been conducted, and therefore methodological weaknesses in existing observational studies limit conclusions about causation.

Data on fetal reproductive and endocrine effects show small, inconsistent associations

Results from observational studies linking prenatal acetaminophen use to abnormalities in the male reproductive tract are inconsistent; some studies have demonstrated small associations with cryptorchidism and reduced anogenital distance, while others have not.5 Furthermore, most studies relied on maternal memory of acetaminophen use in pregnancy, raising the potential for recall bias that may increase observed effect sizes or lead to spurious associations.

Untreated maternal fever has been associated with adverse fetal outcomes

Separating the potential effects of acetaminophen from those of the underlying condition is challenging. Treatment of fever in pregnancy is clinically indicated; in some observational studies, maternal fever was linked to increased risks of neurodevelopmental disorders.6 First-trimester fevers have been linked to congenital abnormalities such as neural tube, heart, and oral cleft defects.7

Counselling on acetaminophen use in pregnancy should emphasize a critical approach to interpreting the data

Current evidence does not indicate a causal link between acetaminophen use in pregnancy and adverse infant outcomes. Clear counselling by clinicians about the limitations of existing observational data can reduce unnecessary anxiety or avoidance of appropriate fever and pain treatment in pregnancy.

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Monday, June 01, 2026

Preprint: Detection of Anti-H5 Antibodies in People with Exposure to Wild Birds in Northern Canada

 

#19,185

Almost exactly 2 years ago - 3 months after the discovery of HPAI H5N1 in U.S. dairy cows - the CDC released the results of their study on Population Immunity to A(H5N1) clade 2.3.3.4b Viruses.  They reported:

CDC analyzed sera (blood) collected from people of all ages in all 10 HHS regions. Blood samples were collected during the 2022-2023 and 2021-2022 flu seasons. These samples were challenged with H5N1 virus to see whether there was an antibody reaction. 

Data from this study suggest that there is extremely low to no population immunity to clade 2.3.4.4b A(H5N1) viruses in the United States.  Antibody levels remained low regardless of whether or not the participants had gotten a seasonal flu vaccination, meaning that seasonal flu vaccination did not produce antibodies to A(H5N1) viruses.

This was in the United States, of course, where exposure to HPAI H5N1 has historically been very low. Over the years we've looked at a number of other seroprevalence studies - particularly in regions with known outbreaks - which have produced slightly different results.

  • In 2004 (see The Thailand Serological Study) 322 poultry farmers (in provinces where H5N1 had been detected) were tested. Researchers found that "no poultry workers had microneutralization titers >80, whereas 7 (2%) had lower titers that did not meet the WHO definition for seropositivity".
  • In May of 2009 (see Cambodian Study Finds Rare Asymptomatic H5N1 Infections) we saw a study published in the Journal of Infectious Diseases on more than 600 members of a Cambodian village where 2 human H5N1 cases were detected in 2006. Antibody titers showed that only 1% (7 of 674) of the villagers tested had contracted, and fought off, the H5N1 virus. A figure much lower than many had expected.
Not unexpectedly, people with direct exposure to infected poultry or livestock tend to have higher detectable levels of HPAI H5 antibodies than the general population. There are a few caveats to serological tests, including:
In other words - while incredibly useful for retrospective investigations - there has always been some degree of ambiguity regarding the results of seroprevalence testing.

All of which brings us to a preprint, published last week, which looks as a small sampling (n=65) of blood samples collected from people (mostly hunters) with exposure to wild birds in Northern Manitoba, Canada. 

The authors reports a ` 7.4% (n=5/68) anti-H5 seroreactivity rate among hunters in Northern Canada'. Some of these hunters had exposure to small mammals as well.  

The authors list some of the limitations to their study, stating:

The relatively small sample size of the study provides limited power for statistical analyses, and given that the study was conducted in a small region of Manitoba, future larger-scale studies are needed to evaluate how commonly people with exposure to wild birds may be infected by H5N1. 

Unfortunately, the durability of the antibody response to H5N1 is unknown, therefore we can only conclude that the five seroreactive individuals have been exposed to the virus at some during their lifetimes, although the durability of antibodies against avian influenza in human populations is unknown. Whether these individuals experienced symptomatic or asymptomatic infections, and whether they would be protected from subsequent re-infection, is also unknown.

I've reproduced the summary and a few excerpts below, but you'll want to follow the link to read this (not-yet peer-reviewed) report in its entirety.  I'll have a bit more after the break. 

Detection of Anti-H5 Antibodies in People with Exposure to Wild Birds in Northern Canada
 Hannah L. Wallace, Morgan Hiebert, Mikayla Hunter, Megan Halbrook, Ryan J. Harrigan, Isaac I. Bogoch, Anne W. Rimoin, Souradet Shaw, Linda Larcombe, Pamela H. Orr, Jason Kindrachuk
doi: https://doi.org/10.64898/2026.05.24.26353994         
Posted May 26, 2026.

        PDF 

Summary

Using a commercially available H5 serology assay, we identified a 7.4% (n=5/68) anti-H5 seroreactivity rate among hunters in Northern Canada. All participants reported close contact with wild birds. 

The Study 

In August 2025 (three months after the 2025 spring goose hunting season), 68 dried blood spot (DBS) samples with matched questionnaires (Appendix 1) were collected from a northern community in Manitoba, Canada. Recruitment was focused on those > 18 years old who were involved in the hunting of birds and/or preparing them (plucking, butchering, food preparation) for consumption.

Some of the participants were also involved in hunting, trapping and handling of mammals (Table 1). Participants were recruited through social media posts and community posters. Participation was voluntary, and included both local community members as well as individuals who were visiting the community for the upcoming fall goose hunting season. Participants were compensated for their involvement in the study. This study was approved by the University of Manitoba Health Research Ethics Board under study HS26941 (H2025-151). 

        (SNIP)

Conclusions

This work indicates that people living and/or hunting in northern Manitoba, Canada have been exposed to H5Nx viruses. Knowledge and concerns about H5N1 among study participants was low, indicating a need for more robust and accessible public health information. Future work including sampling a larger number of individuals and performing longitudinal follow-up to determine how antibody levels change over time would be of significant value. Overall, this work adds to the growing body of literature that aims to understand the true extent of spillovers of avian-origin influenza viruses into humans. 

        (Continue . . . ) 

This isn't the first time we've looked at the potential increased HPAI risk to hunters (and to hunting dogs). Last February we saw Several States Warn On Contact With Wild Birds/Mammals, and the USDA has warned of the risks for several years.

Of course, hunting isn't the only high risk activity.

  • In 2024's Mixed Messaging On HPAI Food Safety - we looked at the risks from the slaughtering of live birds and preparation of raw poultry; especially from birds raised at home or purchased from live markets.

Sadly, the public appears largely unconvinced of the threat from HPAI (see Two Surveys (UK & U.S.) Illustrating The Public's Lack of Concern Over Avian Flu), which almost certainly provides the virus with more opportunities to spread and evolve.  
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Sunday, May 31, 2026

QJM: Avian Influenza in Humans: Virology, Transmission, and Clinical Priorities


Credit WHO

#19,184

While there are no signs that avian influenza is spreading in an efficient or sustained manner between humans, there are concerns that some spillover infections are going unrecognized, and each instance provides with virus with another opportunity to adapt to a human host.

Retrospective antibody testing has shown that some infections are either mild, or subclinical (see JAMA Open: Asymptomatic Human Infections With Avian Influenza A(H5N1) Virus Confirmed by Molecular and Serologic Testing).

Although HPAI H5N1 (clade 2.3.4.4b) is currently viewed as the most worrisome avian flu virus, there are many others, including other H5 subclades (2.3.2.1c or 2.3.2.1a), other H5Nx subtypes, H7 viruses, H9N2, H3N8, and H10Nx

We've also seen reports of atypical presentation (both mild and severe) with avian influenza, along with difficulties in testing some patients, even in a modern hospital setting.

Because of this, we've seen many instances where patients have been hospitalized for days or even weeks before their avian flu infection was finally confirmed.  A few examples:
  • Last April, in Eurosurveillance, we looked at an imported fever/cough case in Italy who initially tested negative for influenza A/B, RSV & COVID, but after a more invasive BAL (Bronchoalveolar lavage), was identified as having H9N2 on the 6th day of his hospitalization. 
While avian flu normally presents as a respiratory infection, we've also seen cases where the symptoms were primarily gastrointestinal, neurological, or subclinical. 

In April of 2025 we saw a preliminary report on a neuroinvasive infection in an 8-y.o. girl (see Vietnam: Ho Chi Minh DOH Reports A Rare H5N1 Encephalitis Case In a Child). While her throat and nose swabs tested negative for influenza A, H5N1 was detected in the patient's cerebrospinal fluid.
As noted by infectious experts, this is a rare case in which the A/H5N1 avian influenza virus damages the central nervous system and does not attack the respiratory tract.
All of which brings us to a narrative review - published this week in the QJM - which argues that avian flu is no longer just a `poultry exposure risk', as its many variants continue to expand both their geographic and (avian & mammalian) host ranges around the globe. 

The opportunities for spillover into humans have increased markedly over the past few years, which makes its important for clinicians to raise their index of suspicion - particularly during times of known outbreaks - even when dealing with atypical presentations or negative test results. 

While this review is `avian flu specific', much of it applies to swine and other novel flu viruses as well. Due to its length, and technical nature, I've only posted some excerpts. Follow the link to read it in its entirety. 

Avian Influenza in Humans: Virology, Transmission, and Clinical Priorities
Nitin Gupta , Anna Smielewska , Jan Felix Drexler , Casandra Bulescu , Marta Mora-Rillo , Aleksandra Barac , Pikka Jokelainen , François-Xavier Lescure , Martin P Grobusch , Sotirios Tsiodras ... Show more
QJM: An International Journal of Medicine, hcag138, https://doi.org/10.1093/qjmed/hcag138
Published:29 May 2026 Article history

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Abstract

Avian influenza continues to evolve as a zoonotic threat with important implications for clinical practice and global health preparedness. Sustained circulation in wild birds, repeated spillover into poultry, and an increasing number of infections across diverse mammalian hosts have reshaped exposure pathways and broadened the risk landscape for human infection. For clinicians, this evolving ecology translates into atypical presentations and increased diagnostic uncertainty. Recent global activity has been characterised by widespread animal outbreaks and the emergence of new transmission interfaces, including occupational exposures and livestock-associated events. Human infections remain largely zoonotic and geographically heterogeneous, with patterns influenced by surveillance intensity, exposure context, and healthcare access.
We synthesise current evidence on the virology, transmission, global epidemiology, clinical manifestations, diagnosis, treatment, and prevention of avian influenza in humans. We highlight evolving mammalian adaptation and changing risk interfaces that complicate risk assessment. Improved clinician awareness, early diagnosis, and integrated One Health surveillance remain central to strengthening preparedness for future influenza threats.
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Clinical Presentation and Diagnosis of Avian Influenza in Humans

Human infection with avian influenza viruses spans a broad clinical spectrum, ranging from asymptomatic infection to severe, rapidly progressive multisystem disease (Table 1) [2,56]. Asymptomatic or subclinical infection has increasingly been recognised through serosurveys and occupational surveillance programmes, indicating that mild infections are likely underdetected outside targeted screening settings [57,58]. 

In a serosurvey of bovine veterinary practitioners in the United States during the 2024 H5 outbreak in dairy cattle, antibodies indicating recent infection were detected in 3 of 150 participants (2%), none of whom reported respiratory or influenza-like symptoms [58]. Similar findings from studies among poultry workers have demonstrated measurable seropositivity in individuals without recognised illness [57]. 

These observations indicate that reliance on clinically apparent cases may underestimate the true burden of zoonotic infections and lead to overestimation of case fatality rates based solely on detected severe cases. 

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Neurological complications, including encephalopathy, encephalitis, seizures, convulsions, and altered consciousness, have been reported in severe H5N1 infection and may occasionally dominate the clinical picture, even in the absence of prominent respiratory disease [69,70].

Human case reports describe acute encephalitis with detectable H5N1 RNA in cerebrospinal fluid, including a child with minimal respiratory symptoms who developed encephalitis complicated by obstructive hydrocephalus, supporting direct central nervous system involvement [71]. Other reported manifestations include diffuse encephalitis, coma, and rapidly progressive neurological deterioration in the setting of severe systemic infection.

Neuropathological and postmortem studies have demonstrated viral antigen and RNA in neurons and glial cells across multiple brain regions, supporting direct neuroinvasion rather than solely secondary inflammatory injury [69]. Experimental studies in ferrets further support this neurotropic potential, showing that H5N1 can invade the brain, often via the olfactory pathway, and may be associated with encephalitis, vasculitis, hemorrhagic lesions, and even subclinical but persistent brain injury [72].

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Conclusion

Avian influenza is ecologically entrenched, globally mobile, and increasingly multi-host. The expansion of H5Nx viruses into previously unafflicted regions, diverse mammalian species, combined with persistent circulation in wild birds and poultry, underscores that the conditions for emergence are continuously present. Apparent epidemiological lulls may reflect surveillance artefacts rather than reduced risk. 

In a world where birds migrate, viruses reassort, and agricultural systems are intensified, preparedness, not prediction, remains the most reliable defence. Strengthening One Health surveillance, ensuring rapid clinical recognition, and maintaining flexible medical countermeasures are essential to prevent avian influenza from becoming the next global pandemic. For clinicians worldwide, recognising avian influenza as an evolving zoonotic interface rather than a rare exotic infection will be central to early detection and response.

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