Monday, July 13, 2026

WHO: Bangladesh Reports 3rd H5N1 Human Infection for 2026

#19,245

In their latest Influenza at the human-animal interface Summary and risk assessment (from 13 June to 7 July 2026) - published over the weekendthe WHO has announced a 3rd H5N1 case in a Bangladeshi child in the past 6 months. 

  • In early June we learned of a 2nd case, a child from Sylhet Division who was hospitalized on March 28th with a clinical diagnosis of measles with bronchopneumonia. The child was discharged on March 31st, but delayed testing by the IEDCR only revealed a positive H5N1 result on April 20th. 

Today, we have another report which - once again - was only fully diagnosed belatedly, and this time the child was only seen as an outpatient.  As with the last case, this case also hails from Sylhet Division. 

On 15 June 2026, Bangladesh notified WHO of one laboratory-confirmed human case of avian influenza A(H5) infection in Bangladesh in a child from Sylhet Division. The case was detected notified through the National Influenza Surveillance, Bangladesh (NISB) platform as an influenza like-illness (ILI) case.
The patient developed respiratory symptoms on 17 May 2026, received outpatient healthcare on 20 May. A clinical sample was collected that day and was received by the Institute of Epidemiology, Disease Control and Research (IEDCR) on 4 June as part of routine surveillance. 
The sample tested positive for influenza A(H5) virus by real-time reverse transcription polymerase chain reaction (RT-PCR) on 11 June. The patient is now in good health and reported no travel history and no history of exposure to poultry.
However, poultry deaths were reported in the area surrounding the patient’s residence. The outbreak investigation team identified and followed close and possible contacts. Samples from some of the close contacts as well as animal and environmental samples were collected for testing for influenza. All contacts remained asymptomatic and all samples tested negative for influenza.
This is the third laboratory-confirmed human case of avian influenza A(H5) reported in Bangladesh in 2026, and the 15th human case of avian influenza A(H5) reported to WHO from Bangladesh since 2008, including two fatal cases, one reported in 2013 and one in 2026

        (Continue . . . )

Sadly, this is a pattern we see far too often, and not just in Bangladesh.  Delayed diagnosis not only endangers the patient's health, it risks unknowingly exposing others to the virus, and delays greatly reduce the effectiveness contact tracing or testing of others who may have been exposed. 

We've seen numerous examples (see here, here, here, and here) of delayed diagnosis of novel flu in hospitalized patients, even here in the United States and in Europe (see H9N2 in Italy). 

Admittedly, novel flu can often present with atypical signs and symptoms, or may be mild or even asymptomaticand not justify hospitalization or comprehensive testing (which may not even be available in some parts of the world). 

Additionally, standard throat swabs sometimes don't yield a positive result, and viral shedding can fluctuate over the course of infection, making false negatives not uncommon. 

Recognizing the problem, in 2024 the ECDC issued guidance for member nations on Enhanced Influenza Surveillance to Detect Avian Influenza Virus Infections in the EU/EEA During the Inter-Seasonal Period.

In that summary, the ECDC pointed out:
Sentinel surveillance systems are important for the monitoring of respiratory viruses in the EU/EEA, but these systems are not designed and are not sufficiently sensitive to identify a newly emerging virus such as avian influenza in the general population early enough for the purpose of implementing control measures in a timely way.

In January 2025 we saw a CDC HAN: Accelerated Subtyping of Influenza A in Hospitalized Patients, which urged immediate, and more thorough subtype testing of suspected flu cases.  

Since these are recommendations, and not mandates, it isn't clear how fine a net we are casting at the local level (see Idaho Health HAN: Consider Avian Influenza A (H5N1) in Patients with Dairy Cattle or Poultry Exposure).

Today's WHO report also summarizes 2 recent H9N2 cases (see chart below), and a novel H3N2v case from Brazil.


Influenza A(H3N2)v, Brazil

On 25 June 2026, Brazil notified PAHO/WHO of a laboratory-confirmed human infection with an influenza A(H3N2)v virus detected in a child in Santa Catarina state. The patient had symptom onset on 12 June 2026 and due to worsening respiratory symptoms, healthcare was sought on 16 June.

The patient was referred for hospital admission with a diagnosis of Severe Acute Respiratory Infection (SARI). Upon admission, an antigen test confirmed influenza A and the patient was placed in a private respiratory isolation room and antiviral treatment was initiated.

The patient was discharged on 19 June.

A nasopharyngeal swab sample was collected on 16 June and sent to the State public health laboratory for real-time RT-PCR. On 18 June, a swine-origin influenza H3 variant was suspected, and the sample was sent to the Laboratory of Respiratory Viruses, Exanthems, Enteroviruses, and Viral Emergencies (LVRE) at the Oswaldo Cruz Institute (Fiocruz/Rio de Janeiro) on 19 June.

Analyses confirmed the presence of an influenza A(H3N2)v virus via molecular testing and genomic sequencing. An investigation by the state and municipality epidemiological surveillance team found that all contacts were asymptomatic before, during and after the child’s illness.

The child's grandfather worked at a swine nursery housing approximately 5,000 animals, though he noted that sanitary barriers were in place. The child frequently visited the grandfather's home and had contact with him several days a week. This is the first human A(H3N2)v infection detected in the Brazil in 2026 and the first case reportedi n the state of Santa Catarina.


In this case, a novel H3 flu virus was suspected in the child after 2 days in the hospital, but was not confirmed until sometime after the patient was discharged (date not explicitly stated)

It takes both planning - and certain amount of luck - to detect novel flu cases in the community, as confirmed cases only represent the very tip of the surveillance and reporting pyramid.  

While there is no evidence that HPAI H5 is spreading efficiently from human-to-human right now, the evidence suggests that it is spilling over into humans more often than we know.  

And even if there is some (as yet, unknown) species barrier that prevents H5 from ever becoming a pandemic, there are plenty of other viruses out there following similar paths. 

Eventually, one of them will get lucky. It's only a matter of time. 

Sunday, July 12, 2026

Updated CDC Surveillance Numbers on Multi-State Cyclosporiasis Outbreak

CDC Surveillance Updated Jul 10th - 843 Confirmed cases


 #19,244

Ten days ago, in Cyclosporiasis Reports: CDC & Michigan DOH, we looked at early reports of a multi-state outbreak of cyclosporiasis, with the CDC reporting 145 cases acquired in the United States between May 1st and June 15th.

At the same time - and not included in the CDC's count - Michigan was reporting an additional 170 cyclosporiasis infections over the previous 9 days.

While fairly common in developing tropical, or sub-tropical countries, Cyclosporiasis – a parasite infection usually acquired through consuming food or water contaminated with Cyclospora cayetanensis - is relatively rare in the United States.

Although it still likely underrepresents the full burden of this outbreak, the CDC's latest update lists 843 confirmed cases, but acknowledges > 1,500 additional reports are under investigation. 

Surveillance of Cyclosporiasis

For Public Health
July 10, 2026

Key points

  • CDC is aware that states are likely to report higher case counts of cyclosporiasis than reflected in CDC data and is working closely with states to update numbers as additional cases are confirmed. Since May 1, 2026, CDC has received reports of 843 confirmed domestic cases of cyclosporiasis and is aware of more than 1,500 cases that require further analysis to confirm the illness as domestically acquired cyclosporiasis. So far this year, multiple states have reported an increase in cases in the last two weeks compared to the same period in 2025.

  • State and federal partners are working together to investigate several outbreaks of cyclosporiasis. Investigations to identify source(s) of illness are ongoing.

  • Cyclosporiasis is a gastrointestinal disease caused by the microscopic parasite Cyclospora.

  • On a regular basis, CDC reports all laboratory-confirmed cases that are received from states. State data may include both probable and confirmed cases, which in turn is likely to reflect a higher case count than the CDC surveillance data because initial case reports have not yet been reported to CDC. CDC does not report probable cases.
Current situation

As of July 9, 2026, 843 cases were reported in people who acquired cyclosporiasis in the United States. Cases were reported by 31 states. These people became sick after eating food in the United States and did not report any travel during the 14 days before they got sick.

Sick people ranged in age from 5 to 88 years, with a median age of 44, and 59% were female. The median illness onset date was June 18, 2026 (range: May 1 – July 5). Of 843 people with information available, 86 were hospitalized. No deaths have been reported.

Multiple jurisdictions have reported an increase of cases in the last two weeks compared to the same period in 2025. We assume a 6-week reporting lag between illness onset and case reporting to CDC; therefore, we anticipate that case counts will continue to rise as data are received.

CDC teams are working diligently to collect, analyze, and provide data at the national level. State health departments may have more timely information about the situation in their jurisdictions.

Local, state, and federal (CDC, FDA) public health authorities are investigating several clusters of cases in more than one state. The numbers reported on this page reflect a total surveillance count of cases across the United States, including clusters of cases currently under traceback investigation by FDA and cases that have not been linked to a common source. Investigations to identify potential sources are ongoing.
In order to help prevent infection, the CDC recommends:

Prevention tips

People can take the following food and vegetable handling recommendations to prevent foodborne illness related to fresh produce:

Wash
  • Wash hands with soap and water before and after handling or preparing raw fruits and vegetables.
Prepare
  • Wash all fruits and vegetables thoroughly under running water before eating, cutting, or cooking.
  • Fruits and vegetables that are labeled "prewashed" do not need to be washed again at home.
  • Scrub firm fruits and vegetables, such as melons and cucumbers, with a clean produce brush.
  • Cut away any damaged or bruised areas on fruits and vegetables before preparing and eating.
Store
  • Refrigerate cut, peeled, or cooked fruits and vegetables as soon as possible (within two hours).

  

Cambodian MOH Announces 5th Human H5N1 Case of 2026

 

#19,243

With thanks for the head's up from @FluTrackers, we have the following announcement from Cambodia's Ministry of Health on their 5th confirmed HPAI H5N1 human infection of 2026 - and 39th in just over 3 years - this time involving a 9-month-old girl from Phnom Penh which was confirmed positive on July 9th.

While most infections in Cambodia have been linked to direct or indirect exposure to infected poultry, there is no mention in today's report a suspected source of infection. The investigation, however, is ongoing. 

The MOH announcement, along with the translation, follow:


(Translation)

Kingdom of Cambodia
Nation Religion King
Ministry of Health

Press Release

On Bird flu case in 9-month-old girl

The Ministry of Health of the Kingdom of Cambodia would like to inform the public that there is 1 case of avian influenza in a 9-month-old girl who was confirmed to be positive for the H5N1 avian influenza virus on 9 July 2026 by the National Institute of Public Health and the Pasteur Institute of Cambodia. The patient is a resident of Prek Ta Kong village, Chak Angre Leu commune, Meanchey district, Phnom Penh. The patient has been placed in isolation at the hospital and is receiving intensive medical care.

The emergency response team of the national and sub-national ministries of health has been collaborating with the teams of the provincial agriculture departments and local authorities at all levels to actively investigate the outbreak of bird flu and respond according to technical methods and protocols, find the source of transmission in both animals and humans, and search for suspected cases and contacts to prevent further transmission in the community, as well as distribute Tamiflu to close contacts and conduct health education campaigns among residents in the affected villages.

The Ministry of Health would like to remind all citizens to always pay attention to and be vigilant about bird flu because H5N1 bird flu continues to threaten the health of our citizens. We would also like to inform you that if you have a fever, cough, runny nose, or difficulty breathing and have a history of contact with sick or dead chickens or ducks within 14 days before the onset of symptoms, do not go to gatherings or crowded places and seek consultation and examination and treatment at the nearest health center or hospital immediately. Avoid delaying this, which puts you at high risk of eventual death.

How it is transmitted: H5N1 bird flu is a type of flu that is usually spread from sick birds to other birds, but it can sometimes be spread from birds to humans through close contact with sick or dead birds. Bird flu in humans is a serious illness that requires prompt hospital treatment. Although it is not easily transmitted from person to person, if it mutates, it can be contagious, just like seasonal flu.

How to prevent:

Do not touch or eat sick or dead chickens and wear gloves and a mask or cover your nose with a scarf before handling chickens for food. Then blanch them in boiling water before plucking their feathers.

1/2

Address: Lot No. 80, Samdech Pen Nut Street (289)
Phone: (+855) 23 885 970
Website: www.moh.gov.kh
Sangkat Boeung Kak 2, Khan Toul Kork, Phnom Penh

Email: info@moh.gov.kh

Telegram: t.me/MOHCambodia

In February of 2023 an older clade of H5N1 (2.3.2.1.x) reemerged in Cambodia's population after a 9 year absence, spilling over into 6 humans in 2023, 10 people in 2024, and 18 people in 2025.

Last October Dr. Erik Karlsson (@eakarlsson.bsky.social‬) from the Institut Pasteur du Cambodge, Phnom Penh, Cambodia, - along with a long list of colleagues - published a brief letter in the NEJM on first 16 cases.

Among them were 4 `clusters' (Father/Daughter, two neighbors, 2 siblings, and 2 cousins living in the same household), 6 fatalities, and 12 cases < 18 years of age.

While human-to-human transmission was considered, the available evidence suggests a `shared' exposure instead, with infected poultry the most likely source of infection.
Most of these recent Cambodian cases have been due to a new reassortment of an older clade of the H5N1 virus (recently renamed 2.3.2.1e) - which appears to be spreading rapidly through both wild birds and local poultry.

Although we usually focus on the more dominant H5 2.3.4.4b clade, these cases remind us that there are other lineages of HPAI H5 still in circulation around the globe (see Viruses: Zoonotic Implications of the Co-Circulation of Clade 2.3.4.4b and 2.3.2.1a H5N1 Avian Influenza Viruses in Nepal in 2023), and each is on their own evolutionary trajectory.

In addition to this very active Cambodia lineage of H5N1, some of the other HPAI H5 contenders we continue to follow include:

Saturday, July 11, 2026

EM&I: Characterization of oseltamivir-resistant A(H5N1) clade 2.3.4.4b, genotype D1.1 variants identified in poultry farms of British Columbia, Canada

Abrupt Shift in H5N1 Genotypes in Wild Birds in US/Canada
Nature https://www.nature.com/articles/s41591-026-04300-1


#19,242

In the fall of 2024 - while we were watching the bovine B3.13 genotype spread in U.S. cattle - a new genotype (D1.1) of H5N1 appeared in Canada and the Pacific Northwest which very quickly became dominant in wild birds and swept eastward across the United States and Canada.

Since then, we've seen roughly 2 dozen confirmed human infections from this D1.1 genotype - several of them severe or fatal (see CDC Statement: First H5 Bird Flu Death Reported in United States) - along with studies suggesting it may better adapted to humans than B3.13 (see J.I.D.: Avian influenza virus A(H5N1) genotype D1.1 is better adapted to human nasal and airway organoids than genotype B3.13).

In early 2025  D1.1 was  detected in dairy cattle in two states (Nevada & Arizona), and later in Wisconsin, further raising concerns over its ability to infect mammals.

When it comes to treating H5N1 infection, Oseltamivir (aka `Tamiflu') remains the overwhelming drug of choice (see below), and makes up > 90% of our stockpiled influenza antiviral armamentarium. 


Previous reports on the incidence of oseltamivir resistance in H5N1 have been fairly reassuring (see 2023's Antiviral Research: Antiviral susceptibility of clade 2.3.4.4b HPAI H5N1 Viruses Isolated From Birds & Mammals in the United States, 2022), but we've seen how quickly that status quo can change. 

Which is why the surprise announcement in February of 2025 that Oseltamivir Resistant H5N1 (Genotype D1.1) had been found On 8 Canadian Poultry Farms in the fall of 2024, raised so many concerns.

In a report from Canada's CFIA and PHAC - the authors described the detection of a (previously) rare H275Y substitution in the neuraminidase (NA) protein of a number of genotype D1.1 isolates, one which is associated with strong resistance to the NA inhibitors oseltamivir and peramivir.

Normally, we only see this mutation appear in a small percentage (1%) of patients receiving antiviral treatment.  Because it is thought to exact a `fitness penalty' on influenza A viruses - limiting forward transmission -  H275Y in the `wild' is fairly rare. 

But over the past few years we've seen evidence of creeping oseltamivir resistance in seasonal H1N1 (FluView Week #20: EOY Review of Increased Detection of Oseltamivir Resistant H1N1 Viruses), along with growing concerns that oseltamivir monotherapy may no longer be the most effective treatment of H5N1.


All of which brings us to a new study, published in Emerging Microbes & Infections, which characterizes the oseltamivir resistant D1.1 viruses detected on 8 Canadian poultry farms in the fall of 2024.  

This is a lengthy, and at times technical, review.  I've posted the abstract and a few excerpts below, but many will want to read the report in its entirety.  I'll have a bit more after the break.

Characterization of oseltamivir-resistant A(H5N1) clade 2.3.4.4b, genotype D1.1 variants identified in poultry farms of British Columbia, Canada

Maxime CochinYacine AbedRobert VendramelliKatrina DionneCatherine BourassaGeneviève Laroche , show all
Article: 2686474 | Received 16 Feb 2026, Accepted 04 Jun 2026, Published online: 08 Jul 2026
 https://doi.org/10.1080/22221751.2026.2686474
ABSTRACT

Highly pathogenic avian influenza A(H5N1) viruses of clade 2.3.4.4b, genotype D1.1, are responsible for widespread outbreaks in poultry and continue to cause sporadic, sometimes severe, human infections. Herein, we characterized a wild-type (WT) influenza A(H5N1) D1.1 isolate (BC-H5N1-WT) and its H275Y neuraminidase (NA) variant (BC-H5N1-H275Y), both of which emerged on farms in British Columbia, Canada, during the fall 2024 outbreak.
In vitro analysis assessed replication kinetics in MDCK cells, with supernatants collected at different days post-infection (p.i.) and titrated by TCID50 and qRT-PCR. Neuraminidase inhibitor (NAI) susceptibility was determined by NA inhibition assays, whereas susceptibility to baloxavir acid (BXA) was evaluated by plaque reduction assay. In vivo virulence was evaluated in BALB/c mice infected with serial 10-fold dilutions of each virus to monitor weight loss and mortality. Viral titers in lungs, brain, nose, kidney, spleen, and heart were quantified at day 4 p.i. The BC-H5N1-WT virus was susceptible to the four antivirals tested, whereas BC-H5N1-H275Y displayed resistance to oseltamivir and peramivir but remained susceptible to zanamivir and BXA.
The BC-H5N1-WT exhibited significantly higher viral replication titers than BC-H5N1-H275Y at all tested time points and showed larger plaque sizes. In mice, BC-H5N1-WT was more virulent with LD50 values of 1.78 × 103 PFUs compared to 8.71 × 104 PFUs for BC-H5N1-H275Y, and produced higher viral titers in lungs and other organs. Despite the reduced fitness of the resistant H5N1 D1.1 variant, its emergence in the absence of viral selection pressure underscores the need for continued surveillance.

        (SNIP)

In October 2024, several chicken farms in the province of BC, Canada, faced an outbreak of HPAIV. Whole genome sequencing confirmed that the virus was an H5N1 virus of the clade 2.3.4.4b [Citation7]. Phylogenetic analysis of the hemagglutinin (HA) and neuraminidase (NA) genes confirmed that the viruses involved were reassortant H5 viruses of clade 2.3.4.4b with an avian NA of N1 subtype from a North American wild bird lineage [Citation7].
Notably, this NA has a longer stalk compared to the truncated NA stalk of traditional HPAI H5N1 strains [Citation8]. Fully Eurasian 2.3.4.4b H5N1 viruses also possess this untruncated (long-stalk) NA, differing from the short-stalk NA common in most pre-2020 highly pathogenic H5N1 strains.
Interestingly, the NA gene from 8 of the 45 sampled poultry farms harboured the well-described H275Y (N1 numbering) substitution that confers high levels of resistance to oseltamivir (OSV) and peramivir (PER), which are influenza NA inhibitors (NAI).
Of note, there was no evidence of OSV or PER use in the related farms that could explain the presence of such H275Y mutants in these animals. Although old H1N1 viruses with the H275Y substitution were associated with a fitness loss [Citation9–11], more recent seasonal and pandemic H1N1 mutant viruses were more fit than the wild-type (WT) virus due to the presence of permissive NA mutations [Citation12–14].

       (SNIP)

It has been well described that the H275Y NA substitution can be selected under OSV pressure either clinically or in experimental in vitro/in vivo procedures. However, to the best of our knowledge, there was no use of OSV in poultry that could explain the emergence of the H275Y NA substitution in BC farms.
  • One possible explanation could be poultry exposure to antivirals in the environment (e.g. via contaminated water near human treatment centers) [Citation40]. 
  • Another possibility is cross-species contamination where the mutation would emerge in humans and spills back into poultry but the only human Canadian case with H5N1 infection so far was not infected by this mutant [Citation6].
  •  A more probable scenario seems to be that the H275Y substitution has emerged spontaneously as influenza viral replication involves an error-prone RNA-dependent RNA polymerase, with random mutations occurring frequently. Such mutation could potentially favour a more optimal balance between HA and NA in some viruses.
OSV is considered the preferred antiviral for the control of a potential influenza pandemic involving avian influenza viruses such as H5N1. Consequently, stockpiles of this compound have been established in several countries worldwide. This study and other observations suggest that it would be unwise not to consider alternatives in the event of the emergence of the H275Y substitution. 
 
This should include the consideration of other antivirals such as BXM, as well as combinations of antivirals with different mechanisms of action, i.e. ZAN (NAI) and BXM (polymerase inhibitor). Also, our findings confirm the need for extensive surveillance studies for influenza drug resistance not restricted to humans.

        (Continue . . . )
 

While the origin of this cluster of H275Y bearing H5N1 viruses remains unclear, the good news is these viruses (at least, back in 2024) showed diminished virulence (in BALB/c mice).

But as we saw with seasonal H1N1 in 2008, `fitness penalties' can be offset by permissive mutations elsewhere in the NA, which is why we follow reports like this one with interest.  

D1.1 isn't the only genotype of concern, and new genotypes will undoubtedly emerge in the future. Most will be evolutionary failures, but the success of B3.13 and D1.1 remind us there are exceptions. 

Even if widespread oseltamivir resistance doesn't emerge, our antiviral stockpile is limited, and we've previously seen problems getting them to patients during the first critical 48 hours of infection (see Sporadic Tamiflu (Oseltamivir) Shortages Reported In U.S. & Canada). 

Once again, our first line of defense will likely rely heavily on NPIs (non-pharmaceutical interventions), like face masks, hand washing, ventilation, staying home while sick, and avoiding crowds.

Which is why I'm recommending that people seriously consider now (see #Natlprep 2025: Personal Pandemic Preparedness) what they will do if another pandemic virus should embark on a new world tour.

Friday, July 10, 2026

Australia Confirms H5N1 in Local Seabird - Confirmed Detections (N=13)

Greater Crested Tern
Link  CC 4.0 Author mattf1996

#19,241

While long expected (see Australia : Biodiversity Council Webinar on HPAI H5 Avian Flu Threat), just three weeks ago Australia reported their first detection of HPAI H5N1 in a migratory bird (brown skua) in Western Australia.

Since then two other states (South Australia & NSW) have reported detections in migratory birds - with the nation's tally standing at 7 as of Monday, July 6th.

Overnight (here in the U.S.) Reuters has reported two new events of import - the first detection of H5N1 in a local seabird in SA, and testing of a dead seal in NSW -  although the most recent governmental summary report mentions neither of them.

It is also worth noting that some of the granular reporting featured in earlier  announcements (exact locations, dates of recovery, suspected cases under investigation, etc.) have recently been replaced by briefer summaries. 

 First, the latest official update. 

June 2026 H5 bird flu detection

As of 8.30pm AEST, 10 July 2026, Australia has 13 confirmed detections of H5 bird flu in wild birds.

There are seven confirmed in Western Australia (WA), five in South Australia (SA) and one in New South Wales (NSW).

There is no evidence of any mass mortality. There is no evidence of infection in poultry or the wider agriculture industry.

The risk to human health remains low.

Australia is well prepared to respond quickly.

If you notice sick or dead birds or other animals, you should not touch them or get too close. Record your location and report it to the 24-hour Emergency Animal Disease Hotline on 1800 675 888.

More information is available in the update below.

While a bit terse, we get some additional detail - including confirmation of the detection in a local seabird - in the following report from Australia's Chief Veterinary Officer: 

H5 bird flu testing updates 

10 July 2026

Attributable to the Australian Chief Veterinary Officer, Dr Beth Cookson:

Testing at CSIRO’s Australian Centre for Disease Preparedness has confirmed four additional detections of H5 high pathogenicity avian influenza (bird flu).

This includes a detection in a greater crested tern, found near Robe, South Australia. This is the first detection of H5 bird flu in an Australian wild non-migratory seabird.

CSIRO’s ACDP has confirmed two additional positive cases in wild migratory seabirds from South Australia. The petrels were found in Port Vincent, Yorke Peninsula and Emu Bay, Kangaroo Island.

CSIRO’s ACDP has also confirmed another positive result in a previously reported suspect petrel from Mullaloo Beach, Perth in Western Australia. Testing remains underway for a further suspect case from a petrel at Horrocks Beach in the Shire of Northampton.

There have now been 12 confirmed or presumed positive detections of H5 bird flu in Australia.

There remains no evidence of any mass mortality events, and there are no detections in poultry or in our agricultural production system.

The risk to human health remains low. 

And lastly we get the following update from Western Australia's Department of Primary Industries and Regional Developmentwhere roughly 100 of  > 1,400 wildlife-related reports have thus far been investigated, producing 7 positive results.

H5 bird flu confirmed on northern WA beaches
Media release

Western Australia has now recorded seven confirmed (or presumed positive) cases of H5 bird flu in individual wild migratory seabirds.

Last updated: 10 July 2026

Western Australia has now recorded seven confirmed (or presumed positive) cases of H5 bird flu in individual wild migratory seabirds.

Testing at CSIRO’s Australian Centre for Disease Preparedness today confirmed the virus in the previously reported suspect positive dead petrel at Mullaloo Beach on the north Perth metropolitan coast.

Another dead petrel previously reported at Horrocks Beach near Northampton was classified as presumed positive with further testing unable to definitively determine H5 bird flu virus through viral sequencing.

It is considered highly likely this bird was infected with H5 bird flu based on the H5 test results, species involved, coastal location and the broader epidemiological picture.

WA is responding to both cases with heightened surveillance in the coastal areas.

Nationally, there have been 13 confirmed or presumed positive results of H5 bird flu in Australia.

This includes 12 wild migratory seabirds, and one confirmed detection announced today in a greater crested tern found near Robe in South Australia. This is the first confirmed detection in an Australian non-migratory seabird.

Importantly, at this time, there is no evidence of any large-scale deaths in wildlife, nor any evidence of infection in poultry or in our agricultural production system

The seven confirmed detections in WA are isolated occurrences and dispersed along a significant length of coastline from east of Esperance to Northampton.

Coastal communities are encouraged to report sick or dead wildlife to the Emergency Animal Disease (EAD) Hotline for assessment.

There has been more than 1400 wildlife-related reports from WA to the hotline since the first confirmed case on 19 June. Of these reports, 228 have been prioritised for further investigation.

To date, a total of 93 negative test results has been recorded across the State.

Each report is carefully reviewed and assessed based on factors such as the species involved, the number of animals affected, the location and the likelihood of disease risk.

Not every report will result in birds being tested or collected, but every report does help inform the understanding of the disease and what is happening in the environment.

People are reminded to avoid handing the animals, record their observations by photo or video and report to the EAD hotline on 1800 675 888.


Based on the previous report of July 6th, the number of wildlife hotline reports has increased by roughly 400 in the past 4 days, while the number of samples tested in WA have risen from 70 to roughly 100. 

Given that 7% of the first 100 tests from WA have come back positive, it is probably safe to say that we are only seeing the tip of the iceberg.

Stay tuned. 

Thursday, July 09, 2026

EFSA: An LPAI H9N2 Mystery



#19,240

A little over a week ago the EFSA published their quarterly avian flu review - which in addition to documenting the last 3 months of Europe's extraordinary 2025-2026 avian flu season - announced the surprise finding of an older, Middle-Eastern/African clade of LPAI H9N2 circulating in Hungary's poultry. 

Despite being clearly zoonotic - LPAI H9N2 is considered a `non-reportable' disease in poultry or wild birds by WOAH (see Terrestrial Animal Code). As a result, there are huge gaps in surveillance and reporting around the world. 

At the same time we've seen a growing number of studies - mostly out of Asia - warning of its growing adaptation to mammalian hosts (see EM&I: Enhanced Replication of a Contemporary Avian Influenza A H9N2 Virus in Human Respiratory Organoids).

Our own CDC lists two lineages (A(H9N2) G1 and A(H9N2) Y280) as having at least some pandemic potential, and several candidate vaccines have been developed.

In terms of risk of emergence, the H9N2
Y280 lineage is ranked higher than H5N1

While there is still much to be learned about them, over the past couple of months we've seen 2 new lineages of LPAI H9N2 described in the literature.

EM&I: A new clade of H9N2 avian influenza virus circulating in Laos

Preprint: Outbreak of H9N2 Avian Influenza Viruses in Lesser Rhea in Peru, June-July 2025

Where H9N2 is endemic (Asia, Africa, the Middle East) attempts at controlling the virus with vaccines have been largely unsuccessful (see J. Virus Erad.: Ineffective Control Of LPAI H9N2 By Inactivated Poultry Vaccines - China).

While most human cases have been reported out of China (see below), this year Europe saw its first (imported) human infection with H9N2 in Italy (see WHO DON: Avian Influenza A(H9N2) - Italy (Ex Senegal))

Reports of LPAI H9N2 in European poultry have been rare, but in this latest report the EFSA describes an outbreak in 7 premises in Hungary.

Apart from these HPAI A(H5N1) outbreaks, Hungary reported the detection of A(H9N2) clade G5.5 virus back in April in 7 establishments keeping chickens (broilers), all of which were located in a single geographical area within one settlement. Increased mortality in one establishment initially raised suspicions of HPAI, however, the birds tested negative for HPAI A(H5) and A(H7) viruses

Tests for infectious bronchitis virus returned positive and pathological examinations revealed tracheitis, presenting with a clinical picture typical of a co-infection (Belkasmi et al., 2020; Regragui et al., 2025). This prompted testing for A(H9N2) virus.

As this specific clade had originally been restricted to countries outside the EU, such as those in the Middle East (Fusaro et al., 2024), poultry workers were interviewed about their travel history; however, no plausible link could be established. 

The source of introduction therefore remained unknown at the time of reporting. All affected establishments were stamped out, cleaned, and disinfected. After 2-3 weeks following repopulation, the birds will be tested again for A(H9N2) virus. Waterfowl flocks present in the affected county were tested for A(H9) virus prior to movement, but all these tests returned negative. 

The report goes on to describe the LPAI H9N2 virus:

Low pathogenic avian influenza A(H9N2) clade G5.5 (CDC, online-a) was identified in two genetically characterised samples collected from commercial poultry establishments in Hungary in April 2026. This clade is circulating in domestic birds in some countries in Africa, the Middle East and West Asia, and has previously never been detected in birds in the EU/EEA. 

Avian influenza A(H9N2) viruses belonging to clade G5.5 have also been reported in sporadic human cases, including Oman and Senegal in 2019, Ghana in 2024, and Italy in March 2026 in a patient who returned from West Africa (Pariani et al., 2026). 

The viruses that are most closely related to the Hungarian strains are A(H9N2) viruses of the same clade that had been circulating in the Middle East one or two decades ago. The long branches and time separating the Hungarian viruses from their progenitors suggest a significant gap of data, making it impossible to determine their origin.

Similarly to the majority of the A(H9N2) viruses of lineages G and B, they possess the HA-Q226L mutation (H3 numbering), which is associated with preferential binding to human-like α2-6-linked sialic acid (SA α2-6) receptors. 


The only recent reports of Clade G5.5 appear to have come from Oman, Senegal, and Ghana, although we are hindered by a general lack of testing, surveillance and reporting.

How it ended up in Hungary - some 4,000km from these locations - is a genuine mystery.  While migratory birds, imported exotic birds, or even human carriage are possible, there is scant evidence to support any conclusion. 

LPAI H9N2 may not be our biggest pandemic threat, but it is far from benign. The fact that H9 has successfully flown under the radar - only to turn up unexpectedly in central Europe - suggests we may want to consider expanding our testing and reporting systems beyond H5 and H7 viruses.