Antivenin‐associated serum sickness in a dog

Lee, Benjamin M; Zersen, Kristin M.; Schissler, Jennifer R.; Sullivan, Louis W.

doi:10.1111/vec.12874

Cited by 7 publications

(16 citation statements)

References 17 publications

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“…There is a possibility that if venom from a different snake species had been used, then different outcomes might have occurred. Antivenom is composed of antibodies to various aspects of snake venom and can include whole immunoglobulin G or antigen‐binding fragments formed after pepsin digestion (F(ab’)2) 2,5–7,9,12,17,23,26,27 . The North American antivenom product contains both the fragment crystallizable region of antibody (Fc) and F(ab’)2 portions of the antibody structure 2,5–7,9,12,17,22,26,27 .…”

Section: Discussionmentioning

confidence: 99%

“…Antivenom is composed of antibodies to various aspects of snake venom and can include whole immunoglobulin G or antigen‐binding fragments formed after pepsin digestion (F(ab’)2) 2,5–7,9,12,17,23,26,27 . The North American antivenom product contains both the fragment crystallizable region of antibody (Fc) and F(ab’)2 portions of the antibody structure 2,5–7,9,12,17,22,26,27 . b Since the Fc portion of the antibody binds complement, it is considered to be the most immunogenic, which has been shown in other Fc‐containing antivenom products 5,9,27 .…”

Section: Discussionmentioning

confidence: 99%

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In vitro evaluation of canine whole blood with the addition of Crotalus atrox (Western Diamondback Rattlesnake) venom and antivenom using thromboelastography

Bailey

Lyon

Gilliam

2022

J Vet Emergen Crit Care

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Objectives: To compare the efficacy of 2 equine-origin antivenom products on correction of coagulation abnormalities noted on thromboelastography (TEG) caused by Crotalus atrox venom in vitro. Design:Prospective in vitro controlled study.Setting: Veterinary teaching hospital. Animals: Six healthy dogs.Interventions: Blood from each dog was used for 4 separate kaolin-activated TEG analyses: A negative control (blood-saline) and positive control (blood-Crotalus atrox venom) were used to assess the dog's normal coagulation and the effect of venom on TEG parameters. Thromboelastographic analyses were then run with blood, venom, and either Argentinian or North American antivenom. All TEG analyses from each dog were compared for efficacy. Measurements and Main Results:The mean R values between the North American antivenom and negative controls were not significantly different (P = 0.681), but were significantly different (P = 0.024) between the Argentinian antivenom and negative controls. The mean fibrinolysis values measured 30 minutes after maximum amplitude achieved between the North American antivenom and negative controls were not significantly different (P = 0.198), but were significantly different (P < 0.001) between the Argentinian antivenom and negative controls. The mean K values between the Argentinian antivenom and negative controls were not significantly different (P = 0.274), but were significantly different (P = 0.043) between the North American antivenom and negative controls. Conclusions:The North American antivenom normalized time to clot formation and fibrinolysis, while the Argentinian antivenom normalized rate of clot formation. Further studies in naturally envenomated patients are necessary to determine if these in vitro results would translate into different clinical outcomes.Abbreviations: F(ab')2, antigen-binding fragments formed after pepsin digestion; Fc, fragment crystallizable region of antibody; K, kinetic time; LY30, fibrinolysis measured 30 minutes after MA achieved; LY60, fibrinolysis measured 60 minutes after MA achieved; MA, maximum amplitude; R, reaction time; TEG, thromboelastography; VICC, venom-induced consumptive coagulopathy.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

In vitro evaluation of canine whole blood with the addition of Crotalus atrox (Western Diamondback Rattlesnake) venom and antivenom using thromboelastography

Bailey

Lyon

Gilliam

2022

J Vet Emergen Crit Care

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“…14,24 However, when an animal is given a whole immunoglobulin product from a different species, antibodies can be found in that animal's bloodstream in 14 to 21 days. 9,21 This raises a question not explored in our study as to which product would be safest to use if a dog is given a fractionated or whole immunoglobulin antivenom product during its initial crotalid envenomation and then has another envenomation episode. We were unaware of any literature indicating a significantly higher reaction rate in dogs or people who have received antivenom on > 1 occasion.…”

Section: Discussionmentioning

confidence: 94%

“…However, the Fc portion also increases the risk of acute type I and delayed type III hypersensitivity reactions. [7][8][9] Two IgG products 10,11 are currently approved by the USDA for use in animals with crotalid envenomation (referred to subsequently as antivenoms C and D).…”

mentioning

confidence: 99%

Retrospective comparison of three antivenoms for the treatment of dogs with crotalid envenomation

Carotenuto¹,

Bergman²,

Ray³

et al. 2021

javma

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OBJECTIVETo retrospectively compare clinical outcomes associated with 3 commercially available antivenom products (2 F[ab']2 products and 1 IgG product) in dogs with crotalid envenomation. ANIMALS282 dogs with evidence of crotalid envenomation treated with antivenom at a single high-volume private emergency facility in southwestern Arizona from 2014 to 2018. PROCEDURESData were collected on all dogs regarding signalment, coagulation test results, snakebite characteristics, type and number of units of antivenom received (1 of 3 products), survival to hospital discharge (yes or no), and complications following discharge. Survival rates and other variables were compared among antivenoms by means of bivariable analyses. RESULTS271 of 282 (96.1%) dogs survived to discharge; 11 (3.9%) were euthanized or died in the hospital. No significant difference in survival rates was found among the 3 antivenom products. Infusion reaction rates were higher for the IgG product than for each F(ab')2 product. A higher percentage of dogs treated with the IgG product (vs either F[ab']2 product) received only 1 unit of antivenom. Variables associated with a lower probability of survival included older age and lower body weight, thoracic (vs other) location of snakebites, and presence of an antivenom infusion reaction. CONCLUSIONS AND CLINICAL RELEVANCEGiven that survival rates were high for all 3 antivenom products, clinicians may consider other factors when selecting an antivenom, such as preference for a fractionated versus whole immunoglobulin product, risk of infusion reaction, cost, shelf life, availability, ease of use and administration, species of crotalids used for antivenom production, approval by federal regulatory bodies, and clinical preference.

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“…38 The prevalence of serum sickness in dogs after administration of antivenom is unknown, but three case reports have been published reporting its occurrence after different antivenoms for viper envenomation in the United States. [41][42][43] In human medicine, there is no consensus regarding the diagnostic criteria for serum sickness; however, it is usually a clinical diagnosis. Australian authors have suggested that clinical signs, risk factors and laboratory data may contribute to a diagnosis.…”

Section: Discussionmentioning

confidence: 99%

Intramyocardial haematoma causing right ventricular outflow obstruction after brown snake (Pseudonaja species) envenomation in a dog

et al. 2020

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A 15‐month‐old, male neutered Staffordshire Bull Terrier cross was presented to its referring veterinarian collapsed and agonal. He was immediately intubated, manually ventilated, and treatment commenced for presumptive snake envenomation with two vials of Tiger/Multi‐Brown Snake Antivenom (minimum 7000 units/vial). The dog was transferred to a referral hospital intubated. Additional diagnostics performed following arrival at the referral hospital included a urine snake venom detection kit test, which was positive for brown snake immunotype. Three additional vials of Tiger/Multi‐Brown Snake Antivenom (minimum 7000 units/vial) were administered until the dog was extubated and able to stand. Venom‐induced consumptive coagulopathy (VICC) was diagnosed based on prolonged clotting times and scleral haemorrhage. Paroxysms of right ventricular outflow tract (RVOT) origin ventricular arrhythmias were treated with lignocaine and sotalol. Four days after presentation, a new‐grade IV/VI systolic heart murmur was auscultated, prompting an echocardiogram. An anechoic and compartmentalised mass measuring 43 mm × 19 mm was visualized within the right ventricular wall at the RVOT, immediately adjacent to the pulmonic valve. The mass was causing a RVOT obstruction. Its appearance was suggestive of an intramyocardial haematoma, most likely secondary to VICC. The dog remained cardiovascularly stable, and treatment consisted of supportive care. Recheck echocardiograms at 2 and 7 weeks after discharge revealed progressive improvement of the intramyocardial mass and resolution of the associated heart murmur. Although intramyocardial haematomas are rare, it should be considered as a differential in dogs that develop a newly diagnosed heart murmur and/or cardiac arrhythmia following brown snake envenomation.

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Antivenin‐associated serum sickness in a dog

Cited by 7 publications

References 17 publications

In vitro evaluation of canine whole blood with the addition of Crotalus atrox (Western Diamondback Rattlesnake) venom and antivenom using thromboelastography

In vitro evaluation of canine whole blood with the addition of Crotalus atrox (Western Diamondback Rattlesnake) venom and antivenom using thromboelastography

Retrospective comparison of three antivenoms for the treatment of dogs with crotalid envenomation

Intramyocardial haematoma causing right ventricular outflow obstruction after brown snake (Pseudonaja species) envenomation in a dog

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