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I wasn’t very quick to write about this because while some incidents of contamination of raw pet food prompt recalls, such contamination is a largely expected event that occurs every day under the radar.

This was also another example of a company ignoring an FDA request to recall raw pet foods in response to contamination, but that too is unfortunately a well known phenomenon when it comes to raw pet food companies.

Listeria contamination adds another dimension, though. Listeria is notorious for contaminating production facilities, particularly those that have suboptimal cleaning, disinfection and maintenance. This can result in widespread and prolonged contamination, with corresponding disease risks. The large number of diets (and over 180 lots) involved in this recall shows the potential scope of Listeria contamination. The company ignoring the problem for some time also likely contributed to unnecessary infections (both detected and undetected).

This recall finally happened months after the US FDA issued a recall request in January 23, 2026 following an owner complaint about their sick dog, and after more reports of dogs on the diets getting sick. The initial recall request was for just 8 lots of various diets, all of which had tested positive for Listeria and other bugs. It’s hard to say how many animals got sick as a result of this incident; Listeria could easily be missed in a dog or cat since it’s not something for which veterinarians typically test.

The company finally responded with a recall on May 22, 2026. The recall affects Raaw Energy diets produced between July 17, 2025 and Dec 23, 2025, as well as “Beef and Turkey Medley” lots produced on March 31, 2026. The notice also states “Some products produced during this timeframe were not tested, and bacterial presence was identified during the same period. As a result, products manufactured within these dates could possibly be affected.” Based on this, combination with the wide date range, I would assume that any diet from this company could be involved at this point. Lack of a positive test for a particular diet doesn’t mean much unless you know how much testing was done.

Ignoring FDA recall requests is an unfortunate pattern with some raw pet food companies. It took months for this company to take action, creating more disease risk for animals and people. I can’t understand why companies are allowed to do this, nor why consumers would continue to purchase from a company that ignores an FDA recall request. If nothing else, you’d think the company would be worried about legal liability if there are further illnesses (especially in people handling the food, or those living with / looking after the dogs), but apparently the short term benefit of ignoring the FDA and continuing to sell contaminated food took precedent.

I’m not going to get into the raw pet food debate (again) here. There’s lots of information in our blog archives, and more information about risk reduction with regard to raw diets can be found on the Worms & Germs Resources – Pets page. Regardless of differences in opinion about the pros and cons of raw diets, I hope we can at least agree on not feeding pets food from companies that ignore food safety problems and contribute to unnecessary disease spread.

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I’ve seen quite a bit of “can your dog or cat get hantavirus?” discussion in media lately, in follow up to the recent cluster of human hantavirus cases associated with a South Atlantic cruise ship. Fortunately, unlike past articles about many other emerging infectious diseases, these have mainly been pretty low key. They’ve highlighted the minimal concern about dogs and cats getting infected and even lower concern that they could infect someone else. Yay.

It is nonetheless important to note is that research on hantavirus in dogs and cats is very limited, so we need to consider “absence of evidence” vs “evidence of absence”. We don’t even know all we need to know about this hantavirus strain (Andes virus) in people; the unique nature of the cruise ship cluster shows this. Animals are much lower down the research priority pecking order.

A few studies have looked at antibodies against hantaviruses in healthy dogs and cats. Finding antibodies means the animal was likely infected at some point and fought off the infection. It doesn’t tell us whether or not they got sick, or whether they could have spread it, but it gives us a basic indication of susceptibility.

These studies tell that a small but appreciable percentage of dogs and cats in areas where hantaviruses are present have evidence of past infection. That’s not overly surprising. They don’t tell us if they got sick or not. If illness caused by hantavirus was really common, we might figure it out based on the clinical cases popping up, but we don’t do a good job identifying rare, sporadic problems, especially in pets, because they’re not routinely tested. I’ve dealt with lots of cases of severe respiratory disease in dogs and cats, and have never tested for hantavirus (maybe we should in some regions, but finding a lab that offers a PCR test for the virus would be the first step). So I’d be wary of dismissing the possibility too quickly, but at the same time it’s not something I’m worried about.

The risk to people posed by infected animals is presumably even lower. We know that people are susceptible to hantaviruses and can get severe disease. Infected people should be more likely to transmit hantaviruses, yet that seems to be really rare, and only a concern with one type of hantavirus (the Andes virus, which was identified in the cruise ship cluster). If dogs and cats are less susceptible to infection in the first place, they likely pose even less risk of transmitting the virus.

Furthermore, we need to remember that not all hantaviruses are the same. There are actually numerous hantaviruses, each with different reservoir hosts and potential issues. We don’t have good data for all the different combinations of hantavirus types and animal species.

While lack of evidence of a problem doesn’t mean there’s no potential problem, it’s encouraging. We have known about hantaviruses for years, and domestic animals have had lots of exposure. Dogs and cats may be at higher risk of exposure than people because they are more likely to catch reservoir hosts (rodents) or root around areas contaminated with rodent urine and feces. Since we’re not seeing suspicious hantavirus cases in dogs and cats, that’s a good sign that the risks are at least low.

BUT we can’t ignore the potential risk altogether. A little common sense is useful to mitigate risks, especially when we don’t know what they are or if they exist. A lot of it is just applying the prevention messaging that is going out to people to other animals.

  • Limit contact with rodents. That is easier said than done for free-roaming dogs and cats, but efforts to keep animals under control and reduce rodent exposure are useful for a bunch of reasons.
  • Reduce rodent access and infestations in households.
  • Take care in areas potentially contaminated with rodent feces and urine. If you’re cleaning out your contaminated shed, maximize ventilation, wear gloves, mask, and eye protection, and wet down surfaces before disturbing them (e.g. sweeping). Also don’t let your dog “help” by shoving his nose in every contaminated corner (or as the case would be with my dog Ozzie, eating everything he can find).

Those are the main things I’d recommend for dogs and cats in areas where hantaviruses are present. Realistically, I’d say the same thing for any other area too, since it’s possible there is unknown hantavirus activity, and hantavirus isn’t the only infectious disease concern when it comes to rodent contact.

Don’t panic over hantavirus, especially when it comes to pets. However, we shouldn’t ignore the potential for animal and interspecies concerns. More surveillance would help determine what the issues really are.

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I got a lot of media questions about hantavirus after the recent cluster of human cases was identified associated with a cruise ship, but those questions were primarily focused on basic facts about virus itself and its general epidemiology. As things have dragged on, there are now more questions about hantavirus and companion animals – not because there are any major issues with pets and this virus, but more likely just because people are getting bored with the usual talking points and are looking for other content.

That said, there are some interesting aspects to consider when it comes to hantavirus and dogs and cats. Pets can be exposed to hantavirus just like people, through contact with reservoir species (i.e. rodents), or their feces, urine or saliva. Cats and dogs are technically at higher risk of exposure in many ways, since they are more likely to have close contact with rodents and to be sniffing around contaminated areas.

I want to start with the key point that the issues with hantavirus in pets are near negligible. I’m going to talk about some areas we should think about with emerging or unusual disease events out of an abundance of caution, not because there’s a major concern with this specific event. So please don’t freak out. Finding that sweet spot between awareness and panic is tough with infectious diseases.

This post will focus on issues to consider specific to the cruise ship cluster. I’ll try to cover some of the more general considerations with hantavirus and pets in another post.

Key point: Despite evidence of human-to-human transmission of this particular hantavirus strain (Andes virus) on the ship, such transmission is still rare. If human-to-human transmission is rare, human-to-pet transmission should be at least as rare, if not even rarer.

Issues with pets and emerging diseases in general revolve around three main concerns:

  1. Pets getting sick (concern for pet health and potential for them to be sources of infection)
  2. Pets getting infected but not sick (no concern for pet health, but bigger to other animals and people to have infectious but apparently healthy animals around us)
  3. Pets acting as vectors of a pathogen whereby they are not infected but can move the virus from place to place (e.g. virus contamination of their haircoats)

We don’t know that any of these are an issue, and they are probably of no concern with this cluster. Infections in dogs and cats are already very rare, and even if infected, the transmission risk from a pet would be very low. But this is also an opportunity to take some basic and practical prevention measures when the risk isn’t well known.

I haven’t seen any reports of dogs being on the ship (e.g. service animals). That removes the highest risk situation with regard to transmission. That leaves us with pets owned by people who have left the ship. Those who have been released from the cruise ship are being monitored, and in some situations tested. Different countries are taking different approaches, but it seems like voluntary quarantine is being used in many places. That focuses primarily on keeping potentially exposed people away from other people. The question I always have with household quarantine is “what about the pets?” This question seems pretty simple, and has come up in the context of various diseases, but rarely do we get an answer.

  • If someone is quarantining in a household, we need to know if they have pets, and if there is a risk to/from the pet for the disease in question. If there is, or if we can’t say there’s no risk, we should treat the animal like a person, i.e. try to keep the quarantined person away from the pet as well. That helps ensure they don’t infect or contaminate the animal, both for the animal’s health and to avoid the risk the pet might then pose to other animals or people.

With other infectious diseases (not likely applicable here), there can also be concerns about the animal acting as a mechanical vector that can lead to indirect transmission, similar to a contaminated surface or object. As I’m writing this, Alice (my cat) is perched next to me. If I have a respiratory virus and touch my face, and then her, I may contaminate her haircoat. If she then visits someone else in the house they pet her a short time later, that could transfer virus to them, even though Alice wasn’t infected. The worst case scenario is I contaminate or infect Alice, and then she goes outside and infects another animal. Then maybe I’ve released the virus into the broader community, or the wildlife population. This was something we were trying to get across when voluntary isolation was used when SARS-CoV-1 emerged in the early 2000s, and then again with SARS-CoV-2 during the COVID-19 pandemic (rarely with any success).

Again, the issues with this hantavirus cluster specifically are very limited and there’s probably no concern:

  • The odds of a person that is quarantining being infected are really low.
  • The odds of an infected person infecting an animal are even lower.
  • The odds of a person being infected, infecting their animal and that animal getting sick or transmitting the virus to someone else approach zero.

So, why are we even talking about it? Good question. We probably know enough about Andes virus to just say “don’t worry.” However, our knowledge of the potential role of pets in a lot of diseases is pretty low, and we can take simple steps to reduce that risk.

My emphasis here is we should default to assuming there could be cross-species transmission issues and apply basic control measures accordingly, unless/until we determine that there’s no need, rather than waiting until we see a problem and then reacting. With Andes virus, a rapid risk assessment could be done to determine the likely risk and the relative certainty of risk, to determine whether or not it is necessary to tell people to isolate from animals too. Despite all our past experiences and recognition of the scope of susceptible species for many emerging diseases, we are still reactionary when it comes to risks to and from animals.

  • Do I want people to worry about their pets if they’ve been exposed? No.
  • Do I want exposed persons to isolate from their pets? Maybe. If they are isolating from people, it makes sense to isolate from their pets. However, if that’s not practical or if the pet is the person’s key emotional support through quarantine, I’d have them quarantine together.
  • Do I want people to fear animals that might have been in contact with an exposed person? No. We’ve seen over-reactions like this in the past.

The issues with hantavirus and most pets are near negligible, but it’s another reminder that the difference between “humans” and “animals” is in our brains. To a virus, we are all just animals of different species, and we all have the potential to be a nice susceptible host.

Carbapenemase-producing Enterobacterales (CPE) is a group of bacteria with resistance to powerful carbapenem antibiotics such as meropenem. They’re also usually resistant to various other antibiotics, which makes them a big concern because treatment options are very limited, and unfortunately the rate of CPE infections in people is increasing rapidly. To treat them, physicians typically need to use one of the limited number of other powerful antibiotics that may still be effective, but the more we have to use these limited drugs, the more resistance to them we’re going get. It’s a cascading problem.

CPE are predominantly an issue in humans, but they can cause infections in animals too, and in a lot of cases the CPE is likely spread from humans to animals. Regardless of the source in each case, the more widely these resistant bacteria are found, the greater the risk they pose to both people and animals.

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The US CDC’s Emerging Infectious Disease journal has posted a podcast on this topic, following up on a recently published study entitled Genetically Similar High-Risk Strains of Carbapenemase-Producing Enterobacterales in Humans and Companion Animals, United States (Xiaoli et al. 2026). Unfortunately, I think we’re going to hear more about CPE in animals in coming years. Information on CPE cases in people in Ontario is available from Public Health Ontario.

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As H5N1 influenza continues to circulate in wild birds, and spillover into a wide range of other birds and mammals, it’s difficult to find the right messaging with regard to the risk of transmission to people.

  • Historically, H5N1 influenza has had a reported mortality rate of 30-50% in people, but it been a lot lower with the strains currently circulating in most parts of the world.
  • Human infections with H5N1 influenza continue to be really rare overall, but they do occur. Generally milder disease doesn’t mean always milder disease, and a small number of fatalities have been reported in the last few years.
  • Spillover of this virus into domestic animals (including poultry, cattle and cats in particular) continues to occur. These spillovers create more risk to people given the closer and more frequent human contact with domestic animals, but surveillance has been limited in household animals such as cats and dogs.

Communicating risks in situations like this is challenging, since we want to raise awareness so people recognize that there is some risk and a need to take basic precautions, but at the same time, we want to make sure there’s no panic and that the risks are dealt with in a reasonable manner. The sweet spot between awareness and paranoia is often tough to find with infectious diseases (as the current cruise ship hantavirus cluster also shows, but that’s another story).

A recent report in CDC’s Morbidity and Mortality Weekly Reports describes a case of suspected cat-to-human transmission of H5N1 influenza in California. It highlights some risks that we’ve been trying to message for a few years now.

  • The good news is the incident didn’t make the person sick (or at least not sick enough that it got reported. The bad news is that there is evidence that tranmission from the cat occurred at all.

The report describes follow-up of people in Los Angeles County who were exposed to cats that got H5N1 influenza from consuming contaminated raw milk or raw diets.

  • There were ultimately nine confirmed feline cases, and ten other suspect cases.
  • 139 people exposed to these cats were monitored for symptoms of flu; of those, 30 developed flu-like illness.
  • 33 people, including 18 of the people who had signs of upper respiratory tract infection, were tested for H5N1 flu by PCR and all were negative, while 36% tested positive for another respiratory virus (mainly human seasonal flu).

PCR testing mostly detects active infection, where the virus is still present. The challenge with this kind of surveillance is that by the time the cats were diagnosed, contacts identified and notified, and testing performed, the virus was likely to be long gone in people (if it was there at all).  Flu infections tend to have a short incubation period (from exposure to onset of illness), and people don’t shed the virus for very long. The median time from exposure to testing in these individuals was 8 days, which is stretching it for flu, no negative results are not surprising, but can’t entirely rule out transmission.

A complementary testing method is looking for antibodies in blood (serology). Antibodies take time to be produced, but they can stay in circulation for a fairly long period of time. So, someone who was infected a few weeks ago would likely be PCR-negative but antibody-positive. The presence of antibodies tells use there was exposure to the virus at some point, but not when. That’s a big limitation of serology in some situations, but in this case where we suspect the risk of exposure to H5N1 flu other than the known contact with the infected cats is very unlikely, finding antibodies in a person is a pretty solid indication that they were infected by the cat.

Twenty-five (25) of the individuals exposed to the infected cats were tested for H5N1 antibodies, and one was positive – a veterinarian, who had no other identified risk of exposure. They didn’t get sick, but they worked on an infected cat without using any respiratory or eye protection (high-risk contact). That makes it a pretty solid presumptive diagnosis of cat-to-human transmission of H5N1 influenza, even though the person was PCR-negative for H5N1 flu when tested 7 days after exposure (so likely missed the viral shedding period).

You might say “they didn’t get sick, so who cares?” At the individual level, that’s fair, but there are broader issues. This case shows that infected cats do pose some degree of risk to people (which we’ve suspected all along). While this person didn’t get sick, the next person might not be so lucky, based on the dose of virus to which they are exposed, their underlying health, and random quirks of disease.

While the H5N1 virus is still not well adapted to people, the more it’s transmitted between mammals, the greater the risk of it adapting to become better able to infect mammals (including people).

We’re also worried about someone with regular human seasonal flu getting exposed to H5N1 flu at the same time. That creates the potential for recombination, whereby the two flu viruses mix together in the same host, potentially creating a new virus strain with the worst parts of both the seasonal flu virus (i.e. easily transmitted between people) and H5N1 flu (a “new” virus to which there is limited individual and population immunity, and potentially could cause more severe illness).  That’s how pandemic viruses emerge. The odds of that happening are low, but the more the viruses mix in different species, the more that risk increases. Here, a reasonable number of people who were exposed to H5N1-infected cats had confirmed seasonal flu infections, so it’s far from a theoretical risk.

Ultimately this report doesn’t really change the current story much, but it’s documentation of something we had assumed would happen. It reinforces the need to take basic infection control precautions around sick cats that have potentially been exposed to H5N1 flu, to take steps to limit exposure of cats to this virus (like keeping them indoors when possible), and to continue surveillance in this and other species.

And as we saw with cat-to-human transmission of SARS-CoV-2 , veterinarians are at the forefront of this risk.

“Doing nothing often leads to the very best of something.” ~Winne the Pooh

I don’t think the beloved wise sage of a bear was thinking about urine when he said that, but we can nonetheless heed the guidance of Winnie the Pooh when it comes to the management of subclinical bacteriuria. Here’s why:

Subclinical bacteriuria (also called asymptomatic bacteriuria in people) is a condition in which bacteria are present in the urine without causing any disease. In the past, this has often been considered something that needs to be treated, but we now know that the bladder isn’t always a sterile environment, and having some bacteria in it isn’t necessarily bad. Bacteria cycle in an out of the bladder, and subclinical bacteriuria is a common (normal) state for some animals (and people). We also now know that it rarely needs to be treated. In humans, the main indications for treatment are pregnancy and treatment prior to undergoing a urological surgical procedure. Unfortunately, it’s often treated unnecessarily (in both people and animals), which can lead to issues with adverse effects of antimicrobials, antimicrobial resistance, unnecessary costs and unnecessary hassles and stress.

When the first edition of the ISCAID antimicrobial use guidelines for urinary tract disease in dogs and cats (2011) was released, many people pushed back at the recommendation to not treat (or even test to look for) subclinical bacteriuria. By the time the second edition of the ISCAID guidelines for diagnosis and management of bacterial urinary tract infections in dogs and cats (2019) was published, there was a lot less resistance to this recommendation, but unnecessary treatment of this condition is still relatively common. As we continue work on the newest update to these guidelines, we hope for even better uptake, but realize that old habits die hard.

Subclinical bacteriuria is still often treated because of habit or fear. We need to focus on a few concepts to move past this out-of-date practice:

  • We treat disease, not culture results.
  • Not all bugs need to die.
  • If a bacterium isn’t bothering my patient, it shouldn’t bother me (with rare exceptions).
  • Doing something isn’t always better than doing nothing (even though we’re hard wired to think we need to do something). Listen to Winnie!

A new study in the Journal of Veterinary Internal Medicine (Le Corre et al, 2026) provides more support for Pooh’s clinical sense. It’s not earth shattering, and it’s not surprising, but it’s a really important part of providing more data help convince clinicians to leave it be.  

The study is entitled Clinical outcomes and association with disease progression and survival of subclinical bacteriuria in cats with chronic kidney disease: a multicenter retrospective study. The researchers looked at 287 cats with chronic kidney disease, which is a population that’s at increased risk for subclinical bacteriuria. All the cats had urine cultures from samples collected by cystocentesis (i.e. using a needle and syringe to inserted directly into the bladder through the body wall to help reduce contamination of the sample), and none had any signs of lower urinary tract disease (e.g. straining to urinate).

  • Bacteria were isolated from the urine of 38% of cats, which is pretty much in line with prior estimates of subclinical bacteriuria in this population. Unsurprisingly, female cats were 5.3 times as likely to have bacteriuria compared to males.
  • Eschericia coli was the most common bacterial isolate, accounting for 68% of positive cultures, followed by Enterococcus (17%), Staphylococcus (5%) and Pseudomonas (5%). Twenty percent (20%) of bacteria were multi-drug resistant (ugh).
  • Eighty-five (85) of the cats with subclinical bacteriuria were treated with antibiotics, of which 41% were treated before antimicrobial susceptibility data were available.

In cats treated with antibiotics, bacteriuria was identified again later on in 62% of them.

  • That’s a key point. It demonstrates that treating the cats didn’t do anything to change their susceptibility to future episodes of bacteriuria, so it’s not surprising it happened again. This highlights the futility of treating this condition. If we eliminate the bacterium in the bladder today, odds are a new one will move in in the near future. The more we treat, the more likely we are to harm the cat (e.g. adverse events from the antimicrobial treatment), and the next time bacteriuria occurs, it may be resistant to our first line drug of choice. If the cat then develops an actual clinical infection that needs antimicrobials, we may have more limited treatment options.

When the researchers looked at 1500 day follow up in these cats, there was no association between subclinical bacteriuria and survival (see graph below). That fits with an earlier study of bacteriuria in senior cats, and with reams of data from human medicine.

Progression of chronic kidney disease was also assessed in 134 cats. There was no difference in percentage of cats that showed progression of disease in the group with subclinical bacteriuria (42%) versus controls (40%). The detection of multiple episodes of subclinical bacteriuria was also not associated with progression of kidney disease.

There was no statistically significant difference between groups in the development of bacterial cystitis, though there was a numerical difference that’s worthy of further investigation That said, an additional question would be whether cats that were treated were more likely to have other complicating factors that were a driver for cystitis. There was also no significant increased risk of pyelonephritis in untreated cats.

All this supports the notion that subclinical bacteriuria is a common and typically benign state. Treatment can sometimes eliminate bacteria, but not always, and when it does, recurrence of bacteriuria is common. It’s possible that treatment would reduce the subsequent risk of bacterial cystitis, but even if there’s a small effect, we need to consider the potential adverse events associated with treatment, especially when treating lots of cats over and over again.

This was the researchers’ conclusion:

…we found no significant association of SBU with survival and disease progression in cats with CKD. Despite antimicrobial treatment of SBU in cats with CKD, urinary sterilization was not achieved in most cases, and progression to bacterial cystitis or pyelonephritis, although infrequent remained possible. Despite the fact that no clear guidelines for the management of SBU in cats with CKD currently exist, our results do not support routine antimicrobial treatment of this condition. Further evidence on the appropriateness of withholding treatment to manage SBU in cats with CKD remain however to be demonstrated before such recommendations can be made.

Image source: https://tommccallum.com/2021/05/21/doing-nothing-often-leads-to-the-very-best-of-something/

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Colorado State University, in partnership with the University of Bristol, is recruiting licensed veterinarians who have encountered at least one case of Feline Infectious Peritonitis (FIP) since 2019 to complete a brief (20 minute) online survey examining clinicians’ experiences and comfort levels with diagnosing FIP and using antiviral therapies for FIP in cats. Please participate if you meet this criterion!

Your participation is voluntary, and your responses will be kept confidential. Insights from this study will help inform the development of future veterinary education resources related to FIP diagnosis and treatment.

IRB#: 7613 (approval date 02/19/2026)

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I’m on the way home from ESCMID Global, a clinical microbiology and infectious disease conference. Although the conference didn’t include much veterinary-specific content, it did include a good collection of abstracts about zoonotic diseases, including a couple about diseases in veterinarians, one of which described an infection with Brucella canis.

I’ve written about B. canis periodically on this blog. While it’s endemic in dogs in many parts of the world, it’s not well studied. Despite being quite common in some dog populations, disease can still be pretty rare. In Ontario, B. canis has been found in numerous commercial dog breeding operations (puppy mills) whose puppies are sold widely, but most of the clinical cases we see are in imported dogs (which makes me wonder if there are differences in virulence between the strains we have here and those that come from abroad).

From a human health standpoint, there’s sometimes a lot of (somewhat misplaced) concern because the Brucella species found in food animals cause a lot of disease in people in areas where they’re endemic. In contrast, B. canis in dogs often flies under the radar, because despite lots of infected dogs, human infections are rare. Last year we published a scoping review of B. canis cases in people (Weese & Weese, Can Vet J 2025), and we were only able to fine reports of 68 human infections. That’s certainly an underestimate of the true number of cases, since many affected people are likely not diagnosed (or misdiagnosed), and not all cases get published. However, when I talk to colleagues in the human health field about this disease, their response is usually “haven’t seen one” or “Brucella what-a?” In other words, Brucella from dogs really isn’t on their radars.

Nonetheless, it’s still important to keep the risk from B. canis in mind, because rare doesn’t mean never, especially for people handling high risk dogs (e.g. imported dogs, puppy mill dogs) and in high risk situations (e.g. assisting dogs with whelping and contact with the associated maternal or fetal fluids or tissues).

There was a nice abstract at ESCMID from the Royal Liverpool University Hospital about a British veterinarian who became infected with B. canis. This bug has gotten increased attention in the UK in recent years, particularly with regard to imported dogs, but it’s still probably not high on the list for most physicians even there.

  • The affected patient was a 36-year-old companion animal veterinarian who had regular contact with dogs of unknown origin and imported dogs. The lead author (Dr. Firas Maghrabi) said this person also had contact with breeding dogs, which further increases the risk of B. canis exposure.
  • Over the course of two weeks, the veterinarian developed forearm blisters, severe back pain, joint pain, and then fever, headache, chest pain, rash and conjunctivitis. After an extensive workup targeting a wide range of infectious diseases, she was ultimately diagnosed with B. canis infection through identification of the bacterium by PCR in blood and cerebrospinal fluid (CSF), and detection of antibodies against B. canis. She was treated with a combination of antibiotics for 6 months, and fortunately fully recovered in the end.

One of the biggest challenges with B. canis in people is that it’s usually not on the radar, and if you don’t test for it, you’re not likely to find it. The only way you’d find it without a targeted test is if the bacterium grew on a blood culture, which generally isn’t very sensitive for something like this. Specific testing for B. canis is needed, and it’s not widely available for people (and antibody tests for the food animal-associated Brucella species won’t detect B. canis).

Education of physicians is obviously needed, but it’s also a bit unrealistic to expect general practitioners to be read up on every oddball infectious disease that’s out there. More realistically, the focus needs to be on getting infectious disease physicians involved in these case, and ensuring those specialists have adequate awareness of B. canis.

The flip side, which is often overlooked, is patient awareness. While I’m sure physicians dread patients who come in with a “Dr. Google” diagnosis as much as veterinarians do, people can still advocate for themselves and raise issues that might otherwise be missed, particularly if they’re aware of high risk exposures that might not be queried in a typical history. People who handle imported dogs or dogs of unknown origin, particularly for any type of reproductive procedure, should be aware of B. canis. They can then play a role in getting it on the radar earlier in the diagnostic process if they’re ill.

I work with imported dogs and assisted with a birthing last week. Is it possible I have Brucella canis?” is a clear and fair question to ask a healthcare provider. For many physicians, their answer may be “I have no idea,” but it’s the starting point to think about it, and consider whether testing or referral to a specialist is indicated.

Words matter. Inconsistency and inaccuracy with terminology can result in misinterpretation, poor communication and creates challenges when discussing cases, interpreting research and developing guidelines.

This has been particularly evident when it comes to urinary tract disease in dogs and cats. For example, “urinary tract infection (UTI)” is a very generic term that has been commonly used to describe everything from bacterial cystitis to subclinical bacteriuria, a positive urine culture, positive urine cytology, pyelonephritis and a few other conditions, or often even indistinct combinations of those. This creates a lot of challenges since those conditions can have vastly different clinical issues. When we’re not speaking the same language, or when we mix completely different diseases into the same bundle, we create the potential for error, misdirection and misunderstanding.

So as part of our ongoing revision of the International Society for Companion Animal Infectious Diseases (ISCAID) 2019 urinary treatment guidelines, we recently completed an initiative to develop consensus-based definitions for these conditions using a broad group of international participants.

  • The guideline field has advanced a lot in recent years. We’re getting past the time where you could just get a few smart people together to create a guideline based on their knowledge and experience. While those past guidelines were often quite good, and they were really important stepping stones, they lacked broad representation, involvement of stakeholders, consideration of biases and had other limitations. The same applies to developing definitions, which requires a more rigorous process to be done right.

We started off with a steering committee of 5 people from 4 countries, then had a review by the ISCAID guideline working group members (19 people), and then two broader rounds of input from 90 people from 19 countries. The goal was to engage a broad range of people with expertise, through multiple rounds of review and suggestions, to arrive at a consensus.

  • All the methodological details of how we came to our definitions are now published online (Weese et al 2026) for anyone that wants to see them. We tried to be as transparent as possible, explaining what was done each round, how and why decisions were made (including some terms/definitions that we abandoned). It wasn’t easy, but I think it yielded some solid results, with a lot of good discussion along the way.

The final definitions and associated footnote are in the images below. For more information and context (and maybe easier reading), check out the complete open-access paper.

Are these definitions perfect? Probably not.

Did we include everyone who might have had useful input? Definitely not.

That said, they’re a step along the way (in the right direction).

As we said in the paper’s conclusion: “Standardisation of terminology is a foundational component of clinical communication, clinical research, surveillance and guideline development. This initiative has allowed for the creation of terms and definitions based on broad stakeholder consensus. The study’s output should assist with ongoing and future efforts to improve the evidence base pertaining to infectious urinary tract disease and foster improved clinical guidance.”

As the weather (slowly and inconsistently) gets nicer here in Ontario, dogs start to go swimming more. My dog, Ozzie (pictured below), is an embarrassment to the Labrador breed as he will not swim, but he’ll happily wade through water, as long as his feet don’t leave the ground (but he still manages to get thoroughly soaked).

It is also the time of year when the question inevitably comes up (yet again): Do topical parasite preventatives need to be re-dosed more frequently in dogs that swim or get bathed over the summer?

No, they don’t. (An easy answer, for once!)

We have lots of options for parasite control in dogs and cats, including oral, topical and injectable products. There are lots of different pros and cons to each, and I won’t wade into that quagmire but here’s the scoop on the topicals:

  • Topical antiparasitics don’t “coat” the animal and stay on the skin or fur; topical is just the route of administration. These products are rapidly absorbed through the skin, and exert their effects through the body, not on the skin’s surface. A lot of of the absorption occurs within a couple of hours of being applied, and the drug can adhere to the skin and haircoat as the rest is absorbed, with peak serum drug levels occurring 2-7 days later. Once the drug is in the skin (even if it’s not yet in the bloodstream), it can’t be washed off.
  • A 2016 study (Kilp et al.) evaluated “repeated intensive shampooing” starting 3 days after administration of a topical parasite preventative, and there was no effect on the ability of the drug to kill fleas or ticks on the dogs. In another study, (Taenzler et al. 2016) researchers “water immersed’” dogs 3, 21, 49 and 77 days after treatment, shampooed them for 6-8 minutes or did nothing (control group). There was no apparent difference in the efficacy of the anti-parasitic treatment between the three groups.

I just checked the labels for a couple products available in Canada: One said to keep the dog out of water for 72 hours after treatment, and another said that exposure to water (including swimming) starting 60 minutes after treatment, or bathing 90 minutes after treatment, doesn’t impact efficacy.

  • I don’t know if the difference is because some products are absorbed quicker than others, some manufacturers are more conservative than others or because the products were simply studied / evaluated differently.
  • It’s important to pay attention to those product labels though. If anything, they’re probably quite conservative, so if they say that the dog can get wet X hours after treatment, I’d follow that guideline, but if the dog gets rained on earlier than that, it’s likely not a problem. If the dog goes for a swim immediately after the product is applied, I’d be concerned the dog would need to be retreated.

In the absence of specific guidance, it’s reasonable to avoid water immersion or bathing for 48-72 hours after treatment; 24 hours is probably lots in most cases, but 48-72 hours gives a bit more margin of safety.

So, while it can take a little bit of planning and attention to make sure you don’t waste a dose of your dog’s topical preventative (particularly for dogs that swim every day), they only need to stay out of the water for a few days, after that swimming or bathing won’t have any detrimental effect on the treatment.