Liver function of mares submitted to <i>Bothrops</i> antigen inoculation for the production of anti-ophidian sérum

Castillo, Mariana N. Del; Ferreira, Camila S.C.; Balaro, Mario F.A.; Castanheira, Patrícia; Almosny, Nadia R.P.; Pinna, Aline E.

doi:10.1590/1678-5150-PVB-7276

ABSTRACT:

Ophidian accidents have been a medical and veterinary challenge. The only treatment available and recommended by the World Health Organization and the Ministry of Health is serotherapy. This study evaluated the liver function of equines submitted to the immunization protocol currently used by the “Instituto Vital Brazil” to produce anti-Bothrops serum. Five equines were evaluated with Bothrops venom inoculation during three immunization cycles. Blood samples were taken for a biochemical test and a liver assessment due to the damage caused to the liver. The biochemical data that presented significant differences in all animals compared to baseline were AST, ALT, GGT, FA, GLDH and serum protein. Creatinine did not change throughout the experiment. The results obtained suggest that liver alterations may occur throughout the three immunization cycles. There is a great need for new studies aimed at broadening knowledge about venom inoculation protocols in serum producer equines and minimizing the adverse effects of immunization.

INDEX TERMS:
Equine; anti-ophidian serum; liver; GLDH

RESUMO:

Acidentes ofídicos têm sido um desafio médico e veterinário. O único tratamento disponível e preconizado pela Organização Mundial da Saúde e pelo Ministério Saúde é a soroterapia. O presente estudo avaliou a função hepática dos equinos submetidos ao protocolo de imunização empregado atualmente pelo Instituto Vital Brazil para produção do soro antibotrópico. Foram avaliados cinco equinos com inoculação de veneno Botrópico durante o período de três ciclos de imunizações. Amostras de sangue foram coletadas para realização de exame bioquímico e avaliação hepática por conta das lesões causadas no fígado. Os dados bioquímicos que apresentaram diferenças significativas, em todos os animais, comparados ao tempo basal, foram AST, ALT, GGT, FA, GLDH e proteína sérica. Creatinina não apresentou alteração ao longo do experimento. Os resultados obtidos sugerem que ao longo dos três ciclos de imunização podem ocorrer alterações hepáticas. Há uma grande necessidade de novos estudos com objetivo de ampliar o conhecimento acerca dos protocolos de inoculação de veneno nos equinos soroprodutores e minimizar os efeitos adversos da imunização.

TERMOS DE INDEXAÇÃO:
Equinos; soro antiofídico; fígado; GLDH

Introduction

Anti-ophidian serotherapy has been used for over 120 years to treat accidents caused by snakes and other venomous animals. In 1894, three researchers began anti-ophidian serotherapy: Albert Calmette (Calmette 1894Calmette A. 1894. L’immunisatin artificielle des animaux contrele venin des serpents, et la thérapeutique expérimentale des morsures venimeuses. Comptes Rendus Soc. Biol. 46(10):120-124.), Césaire Phisalix, and Gabriel Bertrand (Phisalix & Bertrand 1894Phisalix C. & Bertrand G. 1894. Sur la propriété antitoxique du sang des animaux vaccinés contre le venin de vipère. Comptes Rendus Soc. Biol. 46(10):111-113.). These researchers reported on the use of anti-ophidian serum based on the venom of the Naja tripudians, the France Viper, and Pseudechis from Australia.

Technological advances in the field of antivenom production were focused on the processing of hyperimmune plasma and the purification and fractionation of immunoglobulins, while immunization protocols made little progress during this period (Alvarenga et al. 2014Alvarenga L.M., Zahid M., Di Tommaso A., Juste M.O., Aubrey N., Billiald P. & Muzard J. 2014. Engineering venom’s toxin-neutralizing antibody fragments and its therapeutic potential. Toxins, Basel, 6(8):2541-2567. <https://dx.doi.org/10.3390/toxins6082541> <PMid:25153256>
https://doi.org/10.3390/toxins6082541... ). Serums obtained from hyperimmune horse plasma are a mainstay in the treatment of accidents caused by venomous snakes. The production of serum involves the subcutaneous injection of crotalid venoms into horses. Although these injections cause local alterations such as edema and abscesses in a small percentage of animals, systemic alterations have not yet been demonstrated. The venom inoculated into horses is metabolized by the liver and eliminated by the kidneys (Iwanaga & Suzuki 1979Iwanaga S. & Suzuki T. 1979. Enzymes in snake venom, p.61-158. In: Lee C.-Y. (Ed.), Snake Venoms. Vol.52. Springer-Verlag, New York., Mebs & Ownby 1990Mebs D. & Ownby C.L. 1990. Myotoxic components of snake venoms: their biochemical and biological activities. Pharmac. Ther. 48(2):223-236. <https://dx.doi.org/10.1016/0163-7258(90)90081-C> <PMid:2293240>
https://doi.org/10.1016/0163-7258(90)900... ).

There are few studies evaluating hepatic and renal alterations in animals used in the production of antivenoms. The diagnosis of liver disease is made based on clinical signs, laboratory analyses and imaging tests, as well as histopathological examination of a fragment of the organ taken by biopsy (Davoudi et al. 2013Davoudi S.M., Eshagian M. & EdalatiNasab M. 2013. Overview of hepatic disease in large animals. Adv. Bioresearch 4(4):12-20.). Increases in serum concentrations of the enzymes aspartate aminotransferase (AST), sorbitol dehydrogenase (SDH) and glutamate dehydrogenase (GLDH) indicate hepatocyte damage in equines (Lester et al. 2015Lester S.J., Mollat W.H. & Bryant J.E. 2015. Overview of clinical pathology and the horse. Vet. Clin. N. Am., Equine Pract. 31(2):247-268. <https://dx.doi.org/10.1016/j.cveq.2015.04.004> <PMid:26210952>
https://doi.org/10.1016/j.cveq.2015.04.0... ). This study aimed to evaluate the liver function of equines submitted to the immunization protocol currently used by the “Instituto Vital Brazil” (IVB) to produce anti-Bothrops serum.

Materials and Methods

Animal Ethics. The project was approved by the CEUA of the “Instituto Vital Brazil” (IVB) under number 007/2015.

Animals. The experiment used five female equines without a defined breed, ranging in age from 5 to 15 years old, which had not previously been inoculated with poison and housed at the Instituto Vital Brazil (IVB) under semi-intensive management. All the animals were fed in individual troughs and received 4kg of feed a day, 12kg of chopped grass, 50g of mineral supplement and water at will. The mares (n=5) were subjected to three immunization cycles with a mixture of Bothrops venom.

Bothrops venom. The venom used in the immunizations was prepared by mixing five species of the Bothrops genus: B. jararaca (50%), B. jararacussu (12.5%), B. neuwiedi (12.5%), B. moojeni (12.5%), and B. alternatus (12.5%). The mixture was the same as that used in the immunization protocols to obtain the hyperimmune plasma used to produce anti-ophidian serum at the IVB.

Immunization of equines. The first immunization cycle was called baseline immunization and lasted eight weeks, with one inoculation per week. The first inoculation consisted of 5mg of Bothrops venom diluted in 5ml of saline solution plus 5ml of complete Freund’s adjuvant. The second inoculation consisted of 5mg of venom diluted in 5ml of saline solution (8.5%) plus 5ml of montanide adjuvant ISA50V2. The other inoculations (4th to 8th) were of 5mg of Bothrops venom diluted in 10ml of saline.

After a 4-week rest without immunization, the animals were submitted to a second immunization cycle lasting two weeks. In the first week, an inoculation consisting of 6mg of venom diluted in 4ml of saline plus 4ml of montanide adjuvant ISA50V2 was carried out. In the second week, three inoculations were made, 48 hours apart, consisting of 2mg of venom diluted in 8ml of saline. The animals underwent another rest period of four weeks without immunization and were then subjected to the third immunization cycle, which followed the same protocol as the second immunization cycle (Fig.1).

Fig.1.
Three-cycle immunization protocol for Bothrops venom used by the “Instituto Vital Brazil” in equines.

Complementary tests. During the immunization period, blood samples (with and without anticoagulant) were taken once a week and ultrasound scans were carried out every two weeks to assess the liver. For the control, a blood sample was taken, and an ultrasound assessment was made of each equine one week before (week 0) the start of the first immunization cycle. This sample was identified as S0. Thirteen blood samples and seven ultrasound evaluations were obtained from each equine and identified according to the week in which they were collected (S0 to S20).

Blood sample. After local antisepsis, the blood samples were obtained by puncturing the jugular vein, using a vacutainer system (25 X 8mm needles) and siliconized glass tubes for vacuum collection, with a capacity of 5.0ml containing 15% ethylenediamidetetraacetic acid (EDTA) as an anticoagulant. Immediately after collection, the samples were carefully homogenized and stored in a refrigerated container suitable for transport. Then, to perform the biochemical and total protein tests, blood was collected in a sterile 10ml vacuum tube without anticoagulant. The refrigerated blood samples were transported to the Marcilio D. Nascimento Clinical and Molecular Research Laboratory of the Veterinary Faculty of the “Universidade Federal Fluminense” (UFF). The EDTA-containing blood samples taken from the equines at the “Instituto Vital Brazil” Farm, which were submitted to the anti-Bothrops hyperimmunization protocol, were used to carry out laboratory tests included a complete blood count (CBC) consisting of an erythrogram (count of the number of erythrocytes), hemoglobin, globular volume and red blood cell indices: mean corpuscular volume (MCV), mean corpuscular hemoglobin (MCH) and mean corpuscular concentration (MCHC), and leukogram (global count). Blood samples without anticoagulants were used for liver biochemistry tests, measuring the enzymes Aspartate Transaminase Aminotransferase (AST), Alanine Transaminase (ALT), Gamma Glutamyl Transferase (GGT), Alkaline Phosphatase (AF), Glutamate Dehydrogenase (GLDH) and Total Protein. A spectrophotometric or kinetic methodology was adopted, according to the manufacturer’s standards, using automated equipment (Labmax 4000^®, São Paulo, Brazil) and commercial kits (LabTest^®, São Paulo, Brazil).

Ultrasound evaluation. For the ultrasound examination, an ultrasound machine (Sonoscape, model S6V) with a convex transducer with a frequency of 2 to 5MHz was used. Ultrasound evaluations were carried out by dividing the animal’s abdomen into delimited areas called ultrasound windows, which are separated as follows: middle third of the costal arch on the left side between 8° and 13° ICS; middle third of the left costal arch between 12° and 15° ICS; ventral region of the caudal abdomen to the xiphoid cartilage and external; middle third of the costal arch on the right side, between the 10° and 12° ICS. The ultrasound images of the liver were evaluated for morphology, architecture, and contour.

Statistical analysis. The results were analyzed using the Statistical Analysis System (BIOESTAT^® 5.0, Instituto Mamirauá, Amazonas, Brazil). A descriptive analysis was carried out, and the data was tabulated as mean ± standard deviation or frequency (%). All quantitative data was assessed for normality using the Lilliefors test. The analysis of variance (ANOVA) was applied for paired measurements, and means were compared using the Tukey test (when CV ≤30%) or the Student’s LSD T-Test (when CV >30%). Non-normal data was evaluated using the Kruskal-Wallis test, and means were compared using the Dunn test. Categorical data was evaluated using Fisher’s exact test. For all the data, a significant difference was considered when P<0.05.

Results

The physical examination presented no significant alterations, apart from the occurrence of abscesses in the muscles close to the site of venom inoculation, which were more frequent in the weeks of the first immunization cycle compared to the other weeks.

The blood count presented a decrease in erythrocytes in S1 and S4 and an increase in S8. Hemoglobin decreased in S4, rising again in S5, and remaining there until the end of the experiment. The hematocrit, MCV, and MCHC parameters demonstrated no significant changes, unlike the MHC, which showed a decrease in serum values in S13, S14, and S20. There was an increase in leukocyte values in S7 and a peak with values higher than the reference values in S13, remaining high until the end of the experiment.

In biochemical tests, apart from serum albumin and creatinine (Fig.2), there was a time effect (baseline to S20) on serum AST, ALT, GGT, FA and GLDH (P<0.05). Serum AST rose from S5 and remained stable until the end of the study. ALT presented a peak at S3 of the study and then a decrease in its enzymatic activity between S8 and S14 of the study (Fig.3). GGT presented a first peak of serum elevation between S5 and S8 and a second peak between S13 and S20. AF presented higher serum activity at S5 and S20 (Fig.4). The GLDH enzyme presented higher serum activity between S5 and S8 (Fig.5). There was then a decrease in values in the final two weeks (S19 and S20) of the study. There was also an increase in total serum protein values from S5 onwards, which remained stable until the end of the study at S20 (Table 1).

Fig.2.
Evaluation of total protein and serum albumin in equines throughout the experimental period. Total proteins demonstrated an effect of time, with an increase starting at S5 and remaining stable until the end of the study at S20. Albumin, on the other hand, demonstrated that there was no effect of time between baseline (S0) and the last week of collection (S20).

Fig.3.
Evaluation of the serum enzymes Aspartate Transaminase Aminotransferase (AST) and Alanine Transaminase (ALT) in equines throughout the experimental period, demonstrating the effect of time between baseline (S0) and the last week of collection (S20). Serum AST rose from S5 and remained stable until the end of the study. ALT, on the other hand, presented a peak at S3 of the study and then a decrease in its enzymatic activity between S8 and S14.

Fig.4.
Evaluation of serum enzymes Gamma Glutamyl Transferase (GGT) and Alkaline Phosphatase (AF) in equines throughout the experimental period, demonstrating the effect of time between baseline (S0) and the last week of collection (S20). GGT presented a first peak of serum elevation between S5 and S8 and a second peak between S13 and S20. AF presented higher serum activity at S5 and S20.

Fig.5.
Values found for the enzyme Glutamate Dehydrogenase (GLDH) in equines throughout the experimental period, demonstrating the effect of time between baseline (S0) and the last week of collection (S20). The GLDH enzyme presented higher serum activity between S5 and S8. Then, there was a decrease in values in the final two weeks (S19 and S20).

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Table 1.
Mean ± standard deviation of the index evaluated by serum biochemistry at baseline (before the start of the immunization cycle), after the 1st, 2nd and 3rd immunization cycles of the experimental animals

The ultrasound images of the kidneys demonstrated no statistical difference. On the other hand, ultrasound images of the right hepatic lobe presented significant changes in contour in S2 and S8, returning to normal at the end of the experiment and in echotexture, which was heterogeneous in S20 (P<0.05). The left hepatic lobe, on the other hand, presented changes in contour and echogenicity at S4 and S14, respectively (P<0.05).

Discussion

Edema developed near the inoculated area in the process of immunizing the mares, results also found by Sousa et al. (2011)Sousa M.G., Tokarnia C.H., Brito M.F., Reis A.B., Oliveira C.M., Freitas N.F., Oliveira C.H. & Barbosa J.D. 2011. Aspectos clínico-patológicos do envenenamento Botrópico experimental em equinos. Pesq. Vet. Bras. 31(9):773-780. <https://dx.doi.org/10.1590/S0100-736X2011000900009>
https://doi.org/10.1590/S0100-736X201100... , who administered the venoms of Bothrops jararaca, Bothrops jararacussu, Bothrops moojeni, and Bothropoides neuwiedi subcutaneously in six equines. This tumefaction has also been described in both natural cases (Méndez & Riet-Correa 2007Méndez M.D.C. & Riet-Correa F. 2007. Doenças tóxicas: envenamento botrópico, p.31-38. In: Riet-Correa F., Schild A.L., Lemos R.A.A, Borges J.R.J., Mendonça F.S. & Machado M. (Eds), Doenças em Ruminantes e Equinos. Vol.2. 3ª ed. Varela, São Paulo., WHO 2007WHO 2007. Rabies and Envenomings: a neglected public health issue. World Health Organization, Geneva. 32p.) and experimental cases (Soerensen et al. 1995Soerensen B., Barros A.R., Zezza Neto L.Z, Oliveira A.M., Santos R.V., Messias C.V., Silva A.R.C., Capossoli E.A., Cavalcante N.B.C., Vellucci S.C.C., Repetti E., Santos P.C.G., Pacchini C.E. & Alves Junior M. 1995. Aspecto clínico e laboratorial do envenenamento botrópico e crotálico em bovinos. Unimar Ciências, Marília, 4(2):28-33., Caldas et al. 2008Caldas S.A., Tokarnia C.H., França T.N., Brito M.F., Graça F.A.S., Coelho C.D. & Peixoto P.V. 2008. Aspectos clínico-patológicos e laboratoriais do envenenamento experimental por Bothrops alternatus em bovinos. Pesq. Vet. Bras. 28(6):303-312. <https://dx.doi.org/10.1590/S0100-736X2008000600008>
https://doi.org/10.1590/S0100-736X200800... , Aragão et al. 2010Aragão A.P., Tokarnia C.H., Graça F.A.S., França T.N., Coelho C.D., Caldas S.A. & Peixoto P.V. 2010. Envenenamento experimental por Bothropoides jararaca e Bothrops jararacussu em ovinos: aspectos clínico-patológicos e laboratoriais. Pesq. Vet. Bras. 30(9):717-728. <https://dx.doi.org/10.1590/S0100-736X2010000900003>
https://doi.org/10.1590/S0100-736X201000... , Magalhães 2019Magalhães M.M.M. 2019. Ofidismo: manifestações clínicas, diagnóstico e tratamento. Graduação em Medicina, Centro Universitário UNIFACIG, Manhuaçu. 17p.) by snakes of the former Bothrops genus, regardless of the species affected. One probable cause is the intense proteolytic action (metalloproteases) of the venom with a subsequent generalized inflammatory process, causing edema and even local necrosis. According to Castrillón-Estrada et al. (2007)Castrillón-Estrada D.F., Vélez J.G.A., Hernández-Ruiz E.A. & Palacio L.M.A. 2007. Envenenamiento ofídico. Salud Uninorte 23(1):96-111., the onset of symptoms occurs between 10-20 minutes after envenomation with local edema, and the venom of newborn snakes has a greater hemorrhagic, edematous, and lethal effect compared to adult snakes.

At the end of the first immunization cycle (S8), there was an increase in the serum activities of the enzymes AST and GLDH, which, according to Lester et al. (2015)Lester S.J., Mollat W.H. & Bryant J.E. 2015. Overview of clinical pathology and the horse. Vet. Clin. N. Am., Equine Pract. 31(2):247-268. <https://dx.doi.org/10.1016/j.cveq.2015.04.004> <PMid:26210952>
https://doi.org/10.1016/j.cveq.2015.04.0... , indicate hepatocyte damage in equines. In the study by Armengou et al. (2013)Armengou L., Jose-Cunilleras E., Ríos J., Cesarini C., Viu J. & Monreal L. 2013. Metabolic and endocrine profiles in sick neonatal foals are related to survival. J. Vet. Intern Med. 27(3):567-575. <https://dx.doi.org/10.1111/jvim.12064> <PMid:23527872>
https://doi.org/10.1111/jvim.12064... , data was collected on sick foals and the relationship with some biochemical evaluations, and it was observed that foals that did not survive had a higher median plasma GLDH concentration than the survivors, which may be related to acute liver damage. The necropsy revealed mild microscopic liver lesions, such as hemorrhage, inflammatory infiltration, fibrosis, or hepatocellular necrosis, corroborating the elevated GLDH in the foals. The increase in serum AST enzyme activity persisted in both the second and third cycles, as reported by Barbosa et al. (2011)Barbosa J.D., Sousa M.G.S., Tokarnia C.H., Brito M.F., Reis A.S.B., Bomjardim H.A., Lopes C.T.A. & Oliveira C.M.C. 2011. Quadro clínico-patológico do envenenamento crotálico experimental em bubalinos comparado com o de bovinos. Pesq. Vet. Bras. 31(11):967-973. <https://dx.doi.org/10.1590/S0100-736X2011001100005>
https://doi.org/10.1590/S0100-736X201100... , who assessed sensitivity to Crotalus durissus terrificus venom among buffalo and cattle. AST is a leaky enzyme that is found in high concentrations in hepatocytes and skeletal and cardiac muscle cells of all species. It is, therefore, not a liver-specific enzyme, but its elevation can reveal damage to hepatocytes or muscles (Eades 2009Eades S. 2009. Cases of equine hepatic disease (Proceedings). Dvm360®. Available at <Available at https://www.dvm360.com/view/cases-equine-hepatic-disease-proceedings > Accessed on Mar. 2022.
https://www.dvm360.com/view/cases-equine... , Thrall et al. 2014Thrall A.M., Weiser G., Allison R.W. & Campbell T.W. 2014. Hematologia e Bioquímica Clínica Veterinária. 2nd ed. Roca, São Paulo. 688p.).

The increase in serum ALT activity may be related to the muscle damage caused by Bothrops venom, as described in the literature (Castrillón-Estrada et al. 2007Castrillón-Estrada D.F., Vélez J.G.A., Hernández-Ruiz E.A. & Palacio L.M.A. 2007. Envenenamiento ofídico. Salud Uninorte 23(1):96-111.). Albumin presented a reduction from baseline to the end of the first cycle, which was maintained until the end of the third cycle, corroborating with an experiment by Takahira (1996)Takahira R. 1996. Alterações hemáticas e bioquímicas de cães no envenenamento experimental por Bothrops jararaca (Wiedi, 1824) e Bothrops newiedii (Wangler, 1824). Dissertação (Mestrado), Universidade Estadual Paulista, Botucatu, SP., in which Bothrops jararaca venom was inoculated into dogs. The total protein value was high due to the increase in globulin synthesis resulting from the immunization process since globulins represent a group of large proteins and encompass various types of antibody molecules (Mcgowan 2008Mcgowan C. 2008. Clinical pathology in the racing horse: the role of clinical pathology in assessing fitness and performance. Vet. Clin. N. Am., Equine Pract. 24(2):405-421. <https://dx.doi.org/10.1016/j.cveq.2008.03.001> <PMid:18652962>
https://doi.org/10.1016/j.cveq.2008.03.0... ). FA and GGT are induction enzymes considered to be indicators of cholestasis in equines (Lester et al. 2015Lester S.J., Mollat W.H. & Bryant J.E. 2015. Overview of clinical pathology and the horse. Vet. Clin. N. Am., Equine Pract. 31(2):247-268. <https://dx.doi.org/10.1016/j.cveq.2015.04.004> <PMid:26210952>
https://doi.org/10.1016/j.cveq.2015.04.0... ) and presented an increase in serum activity over the three cycles. The increase in this activity was probably due to intrahepatic causes because of the inoculation of the antigen in the immunization process.

According to Belluomini et al. (1982)Belluomini H.E., Araujo P., Rosenfeld G., Leinz F.F. & Birgel E.H. 1982. Symptomatologie der experimentellen Crotalustoxin-Vergiftung bei Rindern, die einer spezifischen Serumtherapie unterworfen wurden. Dtsch. Tierärztl. Wochenschr. 89(11):444-448. <PMid:6756867>, cattle react most sensitively to snake venom, followed by equines, ovines, goats, canines, and swine. According to Rosenfeld (1971)Rosenfeld G. 1971. Symptomatology, pathology and treatment of snake bites in South America, p.345-384. In: Bücherl W. & Buckley E.E. (Ed.), Venomous Animals and their Venoms. Vol.2. Venomous Vertebrates. Academic Press, New York., carnivores seem to be more resistant to ophidian venoms than other animals, but the cat is resistant to Bothrops venom (proteolytic and coagulant) and very sensitive to the venom of South American Crotalus spp.; the hamster is more resistant than the cat to crotalic venom.

The results of the hematological tests showed normochromic normocytic anemia and persistent thrombocytopenia, corroborating the findings of Sousa et al. (2011)Sousa M.G., Tokarnia C.H., Brito M.F., Reis A.B., Oliveira C.M., Freitas N.F., Oliveira C.H. & Barbosa J.D. 2011. Aspectos clínico-patológicos do envenenamento Botrópico experimental em equinos. Pesq. Vet. Bras. 31(9):773-780. <https://dx.doi.org/10.1590/S0100-736X2011000900009>
https://doi.org/10.1590/S0100-736X201100... , probably caused by the exploratory bleeding process during the second and third immunization cycles. Oliveira et al. (2004)Oliveira N.J.F., Ribeiro E.L., Silva Júnior P.G.P., Lago L.A., Lucia M. & Melo M.M. 2004. Bovine blood profile after Bothrops alternatus envenomation. 8º Congresso da Sociedade Brasileira de Toxinologia, Symposium of the Pan American Section of the International Society on Toxinology. Angra dos Reis, RJ. (Resumo) found changes in the blood profile characterized by leukocytosis in five cows inoculated with Bothrops venom, similar to the findings of this experiment. Otero et al. (1992)Otero R., Tobbn G.S., Gómez L.F., Osorio R., Valderrama R., Hoyos D., Urreta E., Molina S. & Arboleda J.J. 1992. Accidente ofidico en Antioquia y choco. Aspectos clinicos y epidemiologicos (marzo de 1989-febrero de 1990). Acta Med. Colomb. 17(4):229-249. and Cardoso et al. (2009)Cardoso J.L.C., França F.O.S., Wen F.H., Malaque C.M.S. & Haddad Jr. V. 2009. Animais Peçonhentos no Brasil. 2ª ed. Sarvier, São Paulo. 488p. cited leukocytosis as a typical laboratory finding in human crotalic envenomations. Magalhães (2019)Magalhães M.M.M. 2019. Ofidismo: manifestações clínicas, diagnóstico e tratamento. Graduação em Medicina, Centro Universitário UNIFACIG, Manhuaçu. 17p. also reported the presence of thrombocytopenia and leukocytosis with left-shifted neutrophilia and mild anemia in humans in the first few hours after the bite. In a case report, Tolentino et al. (2019)Tolentino L.H.O., Tolentino M.L.D.L., Assis D.M., Firmino M.O., Benvenutti M.E.M., Miranda Neto E.G., Dantas A.F.M. & Vaz A.F.M. 2019. Caracterização clínica, laboratorial e patológica de equino naturalmente acometido por acidente botrópico. Pubvet 13(4):1-8. <https://dx.doi.org/10.31533/pubvet.v13n4a309.1-8>
https://doi.org/10.31533/pubvet.v13n4a30... observed the presence of liver coagulation disorders (thrombocytopenia, hemorrhage, and increased blood coagulation time; decrease in albumin and globulin) and muscle damage (considerable increase in lactate dehydrogenase and creatine kinase), partially corroborating the findings of our experiment.

It was noted that the ultrasound examination was important for the early detection of alterations in the liver parenchyma, even in the absence of changes in biochemical tests, in agreement with the reports described by Mamprim et al. (1997)Mamprim M.J., Rocha N.S., Muniz L.M.R., Vulcano L.C. & Leal A.C.R. 1997. Imagem ultra-sonográfica de metástase abdominal de tumor venéreo transmissível: relato de caso. Anais XIX Congresso Brasileiro de Clínicos Veterinários de Pequenos Animais, Curitiba, PR, p.44. (Resumo) in the experiment with dogs. The lack of literature on hepatic ultrasound examinations, especially in equines, makes it difficult to compare with the present study and determines the importance of our ultrasound findings demonstrating suggestive alterations of an acute condition. It is, therefore, understood that ultrasound is essential for identifying abnormalities in the liver parenchyma at an early stage.

Conclusion

Significant serum biochemical alterations are detected in equines inoculated with Bothrops venom even in the absence of symptoms, which may suggest acute lesions throughout the three immunization cycles. There is an increase in the enzymatic activity of AST, GLDH, GGT and FA throughout the immunization process, which suggests hepatotoxicity action in equines. Total serum proteins also rise as a result of the production of immunoglobulins. The ultrasound images show changes in the integrity of the liver and kidney over the three immunization cycles evaluated. When correlating the results of the laboratory tests with the ultrasound images, it can be seen that both present alterations from the first immunization cycle, such as anemia and irregular liver contour. Thus, due to animal welfare issues and tissue damage resulting from immunization in equines, more studies are needed on Bothrops venom inoculation protocols in order to minimize the adverse effects of immunization.

Acknowledgments

This research was supported by the “Coordenação de Aperfeiçoamento de Pessoal de Nível Superior” (CAPES) and a partnership with the “Instituto Vital Brazil”.

References

Alvarenga L.M., Zahid M., Di Tommaso A., Juste M.O., Aubrey N., Billiald P. & Muzard J. 2014. Engineering venom’s toxin-neutralizing antibody fragments and its therapeutic potential. Toxins, Basel, 6(8):2541-2567. <https://dx.doi.org/10.3390/toxins6082541> <PMid:25153256>
» https://doi.org/10.3390/toxins6082541
Aragão A.P., Tokarnia C.H., Graça F.A.S., França T.N., Coelho C.D., Caldas S.A. & Peixoto P.V. 2010. Envenenamento experimental por Bothropoides jararaca e Bothrops jararacussu em ovinos: aspectos clínico-patológicos e laboratoriais. Pesq. Vet. Bras. 30(9):717-728. <https://dx.doi.org/10.1590/S0100-736X2010000900003>
» https://doi.org/10.1590/S0100-736X2010000900003
Armengou L., Jose-Cunilleras E., Ríos J., Cesarini C., Viu J. & Monreal L. 2013. Metabolic and endocrine profiles in sick neonatal foals are related to survival. J. Vet. Intern Med. 27(3):567-575. <https://dx.doi.org/10.1111/jvim.12064> <PMid:23527872>
» https://doi.org/10.1111/jvim.12064
Barbosa J.D., Sousa M.G.S., Tokarnia C.H., Brito M.F., Reis A.S.B., Bomjardim H.A., Lopes C.T.A. & Oliveira C.M.C. 2011. Quadro clínico-patológico do envenenamento crotálico experimental em bubalinos comparado com o de bovinos. Pesq. Vet. Bras. 31(11):967-973. <https://dx.doi.org/10.1590/S0100-736X2011001100005>
» https://doi.org/10.1590/S0100-736X2011001100005
Belluomini H.E., Araujo P., Rosenfeld G., Leinz F.F. & Birgel E.H. 1982. Symptomatologie der experimentellen Crotalustoxin-Vergiftung bei Rindern, die einer spezifischen Serumtherapie unterworfen wurden. Dtsch. Tierärztl. Wochenschr. 89(11):444-448. <PMid:6756867>
Caldas S.A., Tokarnia C.H., França T.N., Brito M.F., Graça F.A.S., Coelho C.D. & Peixoto P.V. 2008. Aspectos clínico-patológicos e laboratoriais do envenenamento experimental por Bothrops alternatus em bovinos. Pesq. Vet. Bras. 28(6):303-312. <https://dx.doi.org/10.1590/S0100-736X2008000600008>
» https://doi.org/10.1590/S0100-736X2008000600008
Calmette A. 1894. L’immunisatin artificielle des animaux contrele venin des serpents, et la thérapeutique expérimentale des morsures venimeuses. Comptes Rendus Soc. Biol. 46(10):120-124.
Cardoso J.L.C., França F.O.S., Wen F.H., Malaque C.M.S. & Haddad Jr. V. 2009. Animais Peçonhentos no Brasil. 2ª ed. Sarvier, São Paulo. 488p.
Castrillón-Estrada D.F., Vélez J.G.A., Hernández-Ruiz E.A. & Palacio L.M.A. 2007. Envenenamiento ofídico. Salud Uninorte 23(1):96-111.
Davoudi S.M., Eshagian M. & EdalatiNasab M. 2013. Overview of hepatic disease in large animals. Adv. Bioresearch 4(4):12-20.
Eades S. 2009. Cases of equine hepatic disease (Proceedings). Dvm360^® Available at <Available at https://www.dvm360.com/view/cases-equine-hepatic-disease-proceedings > Accessed on Mar. 2022.
» https://www.dvm360.com/view/cases-equine-hepatic-disease-proceedings
Iwanaga S. & Suzuki T. 1979. Enzymes in snake venom, p.61-158. In: Lee C.-Y. (Ed.), Snake Venoms. Vol.52. Springer-Verlag, New York.
Lester S.J., Mollat W.H. & Bryant J.E. 2015. Overview of clinical pathology and the horse. Vet. Clin. N. Am., Equine Pract. 31(2):247-268. <https://dx.doi.org/10.1016/j.cveq.2015.04.004> <PMid:26210952>
» https://doi.org/10.1016/j.cveq.2015.04.004
Magalhães M.M.M. 2019. Ofidismo: manifestações clínicas, diagnóstico e tratamento. Graduação em Medicina, Centro Universitário UNIFACIG, Manhuaçu. 17p.
Mamprim M.J., Rocha N.S., Muniz L.M.R., Vulcano L.C. & Leal A.C.R. 1997. Imagem ultra-sonográfica de metástase abdominal de tumor venéreo transmissível: relato de caso. Anais XIX Congresso Brasileiro de Clínicos Veterinários de Pequenos Animais, Curitiba, PR, p.44. (Resumo)
Mcgowan C. 2008. Clinical pathology in the racing horse: the role of clinical pathology in assessing fitness and performance. Vet. Clin. N. Am., Equine Pract. 24(2):405-421. <https://dx.doi.org/10.1016/j.cveq.2008.03.001> <PMid:18652962>
» https://doi.org/10.1016/j.cveq.2008.03.001
Mebs D. & Ownby C.L. 1990. Myotoxic components of snake venoms: their biochemical and biological activities. Pharmac. Ther. 48(2):223-236. <https://dx.doi.org/10.1016/0163-7258(90)90081-C> <PMid:2293240>
» https://doi.org/10.1016/0163-7258(90)90081-C
Méndez M.D.C. & Riet-Correa F. 2007. Doenças tóxicas: envenamento botrópico, p.31-38. In: Riet-Correa F., Schild A.L., Lemos R.A.A, Borges J.R.J., Mendonça F.S. & Machado M. (Eds), Doenças em Ruminantes e Equinos. Vol.2. 3ª ed. Varela, São Paulo.
Oliveira N.J.F., Ribeiro E.L., Silva Júnior P.G.P., Lago L.A., Lucia M. & Melo M.M. 2004. Bovine blood profile after Bothrops alternatus envenomation. 8º Congresso da Sociedade Brasileira de Toxinologia, Symposium of the Pan American Section of the International Society on Toxinology. Angra dos Reis, RJ. (Resumo)
Otero R., Tobbn G.S., Gómez L.F., Osorio R., Valderrama R., Hoyos D., Urreta E., Molina S. & Arboleda J.J. 1992. Accidente ofidico en Antioquia y choco. Aspectos clinicos y epidemiologicos (marzo de 1989-febrero de 1990). Acta Med. Colomb. 17(4):229-249.
Phisalix C. & Bertrand G. 1894. Sur la propriété antitoxique du sang des animaux vaccinés contre le venin de vipère. Comptes Rendus Soc. Biol. 46(10):111-113.
Rosenfeld G. 1971. Symptomatology, pathology and treatment of snake bites in South America, p.345-384. In: Bücherl W. & Buckley E.E. (Ed.), Venomous Animals and their Venoms. Vol.2. Venomous Vertebrates. Academic Press, New York.
Soerensen B., Barros A.R., Zezza Neto L.Z, Oliveira A.M., Santos R.V., Messias C.V., Silva A.R.C., Capossoli E.A., Cavalcante N.B.C., Vellucci S.C.C., Repetti E., Santos P.C.G., Pacchini C.E. & Alves Junior M. 1995. Aspecto clínico e laboratorial do envenenamento botrópico e crotálico em bovinos. Unimar Ciências, Marília, 4(2):28-33.
Sousa M.G., Tokarnia C.H., Brito M.F., Reis A.B., Oliveira C.M., Freitas N.F., Oliveira C.H. & Barbosa J.D. 2011. Aspectos clínico-patológicos do envenenamento Botrópico experimental em equinos. Pesq. Vet. Bras. 31(9):773-780. <https://dx.doi.org/10.1590/S0100-736X2011000900009>
» https://doi.org/10.1590/S0100-736X2011000900009
Takahira R. 1996. Alterações hemáticas e bioquímicas de cães no envenenamento experimental por Bothrops jararaca (Wiedi, 1824) e Bothrops newiedii (Wangler, 1824). Dissertação (Mestrado), Universidade Estadual Paulista, Botucatu, SP.
Thrall A.M., Weiser G., Allison R.W. & Campbell T.W. 2014. Hematologia e Bioquímica Clínica Veterinária. 2nd ed. Roca, São Paulo. 688p.
Tolentino L.H.O., Tolentino M.L.D.L., Assis D.M., Firmino M.O., Benvenutti M.E.M., Miranda Neto E.G., Dantas A.F.M. & Vaz A.F.M. 2019. Caracterização clínica, laboratorial e patológica de equino naturalmente acometido por acidente botrópico. Pubvet 13(4):1-8. <https://dx.doi.org/10.31533/pubvet.v13n4a309.1-8>
» https://doi.org/10.31533/pubvet.v13n4a309.1-8
WHO 2007. Rabies and Envenomings: a neglected public health issue. World Health Organization, Geneva. 32p.

Master’s research with CAPES support.

Publication Dates

Publication in this collection
31 May 2024
Date of issue
2024

History

Received
20 Oct 2023
Accepted
19 Dec 2023

This is an open-access article distributed under the terms of the Creative Commons Attribution License

[1] Alvarenga L.M., Zahid M., Di Tommaso A., Juste M.O., Aubrey N., Billiald P. & Muzard J. 2014. Engineering venom’s toxin-neutralizing antibody fragments and its therapeutic potential. Toxins, Basel, 6(8):2541-2567. <https://dx.doi.org/10.3390/toxins6082541> <PMid:25153256>
» https://doi.org/10.3390/toxins6082541

[2] Aragão A.P., Tokarnia C.H., Graça F.A.S., França T.N., Coelho C.D., Caldas S.A. & Peixoto P.V. 2010. Envenenamento experimental por Bothropoides jararaca e Bothrops jararacussu em ovinos: aspectos clínico-patológicos e laboratoriais. Pesq. Vet. Bras. 30(9):717-728. <https://dx.doi.org/10.1590/S0100-736X2010000900003>
» https://doi.org/10.1590/S0100-736X2010000900003

[3] Armengou L., Jose-Cunilleras E., Ríos J., Cesarini C., Viu J. & Monreal L. 2013. Metabolic and endocrine profiles in sick neonatal foals are related to survival. J. Vet. Intern Med. 27(3):567-575. <https://dx.doi.org/10.1111/jvim.12064> <PMid:23527872>
» https://doi.org/10.1111/jvim.12064

[4] Barbosa J.D., Sousa M.G.S., Tokarnia C.H., Brito M.F., Reis A.S.B., Bomjardim H.A., Lopes C.T.A. & Oliveira C.M.C. 2011. Quadro clínico-patológico do envenenamento crotálico experimental em bubalinos comparado com o de bovinos. Pesq. Vet. Bras. 31(11):967-973. <https://dx.doi.org/10.1590/S0100-736X2011001100005>
» https://doi.org/10.1590/S0100-736X2011001100005

[5] Belluomini H.E., Araujo P., Rosenfeld G., Leinz F.F. & Birgel E.H. 1982. Symptomatologie der experimentellen Crotalustoxin-Vergiftung bei Rindern, die einer spezifischen Serumtherapie unterworfen wurden. Dtsch. Tierärztl. Wochenschr. 89(11):444-448. <PMid:6756867>

[6] Caldas S.A., Tokarnia C.H., França T.N., Brito M.F., Graça F.A.S., Coelho C.D. & Peixoto P.V. 2008. Aspectos clínico-patológicos e laboratoriais do envenenamento experimental por Bothrops alternatus em bovinos. Pesq. Vet. Bras. 28(6):303-312. <https://dx.doi.org/10.1590/S0100-736X2008000600008>
» https://doi.org/10.1590/S0100-736X2008000600008

[7] Calmette A. 1894. L’immunisatin artificielle des animaux contrele venin des serpents, et la thérapeutique expérimentale des morsures venimeuses. Comptes Rendus Soc. Biol. 46(10):120-124.

[8] Cardoso J.L.C., França F.O.S., Wen F.H., Malaque C.M.S. & Haddad Jr. V. 2009. Animais Peçonhentos no Brasil. 2ª ed. Sarvier, São Paulo. 488p.

[9] Castrillón-Estrada D.F., Vélez J.G.A., Hernández-Ruiz E.A. & Palacio L.M.A. 2007. Envenenamiento ofídico. Salud Uninorte 23(1):96-111.

[10] Davoudi S.M., Eshagian M. & EdalatiNasab M. 2013. Overview of hepatic disease in large animals. Adv. Bioresearch 4(4):12-20.

[11] Eades S. 2009. Cases of equine hepatic disease (Proceedings). Dvm360^® Available at <Available at https://www.dvm360.com/view/cases-equine-hepatic-disease-proceedings > Accessed on Mar. 2022.
» https://www.dvm360.com/view/cases-equine-hepatic-disease-proceedings

[12] Iwanaga S. & Suzuki T. 1979. Enzymes in snake venom, p.61-158. In: Lee C.-Y. (Ed.), Snake Venoms. Vol.52. Springer-Verlag, New York.

[13] Lester S.J., Mollat W.H. & Bryant J.E. 2015. Overview of clinical pathology and the horse. Vet. Clin. N. Am., Equine Pract. 31(2):247-268. <https://dx.doi.org/10.1016/j.cveq.2015.04.004> <PMid:26210952>
» https://doi.org/10.1016/j.cveq.2015.04.004

[14] Magalhães M.M.M. 2019. Ofidismo: manifestações clínicas, diagnóstico e tratamento. Graduação em Medicina, Centro Universitário UNIFACIG, Manhuaçu. 17p.

[15] Mamprim M.J., Rocha N.S., Muniz L.M.R., Vulcano L.C. & Leal A.C.R. 1997. Imagem ultra-sonográfica de metástase abdominal de tumor venéreo transmissível: relato de caso. Anais XIX Congresso Brasileiro de Clínicos Veterinários de Pequenos Animais, Curitiba, PR, p.44. (Resumo)

[16] Mcgowan C. 2008. Clinical pathology in the racing horse: the role of clinical pathology in assessing fitness and performance. Vet. Clin. N. Am., Equine Pract. 24(2):405-421. <https://dx.doi.org/10.1016/j.cveq.2008.03.001> <PMid:18652962>
» https://doi.org/10.1016/j.cveq.2008.03.001

[17] Mebs D. & Ownby C.L. 1990. Myotoxic components of snake venoms: their biochemical and biological activities. Pharmac. Ther. 48(2):223-236. <https://dx.doi.org/10.1016/0163-7258(90)90081-C> <PMid:2293240>
» https://doi.org/10.1016/0163-7258(90)90081-C

[18] Méndez M.D.C. & Riet-Correa F. 2007. Doenças tóxicas: envenamento botrópico, p.31-38. In: Riet-Correa F., Schild A.L., Lemos R.A.A, Borges J.R.J., Mendonça F.S. & Machado M. (Eds), Doenças em Ruminantes e Equinos. Vol.2. 3ª ed. Varela, São Paulo.

[19] Oliveira N.J.F., Ribeiro E.L., Silva Júnior P.G.P., Lago L.A., Lucia M. & Melo M.M. 2004. Bovine blood profile after Bothrops alternatus envenomation. 8º Congresso da Sociedade Brasileira de Toxinologia, Symposium of the Pan American Section of the International Society on Toxinology. Angra dos Reis, RJ. (Resumo)

[20] Otero R., Tobbn G.S., Gómez L.F., Osorio R., Valderrama R., Hoyos D., Urreta E., Molina S. & Arboleda J.J. 1992. Accidente ofidico en Antioquia y choco. Aspectos clinicos y epidemiologicos (marzo de 1989-febrero de 1990). Acta Med. Colomb. 17(4):229-249.

[21] Phisalix C. & Bertrand G. 1894. Sur la propriété antitoxique du sang des animaux vaccinés contre le venin de vipère. Comptes Rendus Soc. Biol. 46(10):111-113.

[22] Rosenfeld G. 1971. Symptomatology, pathology and treatment of snake bites in South America, p.345-384. In: Bücherl W. & Buckley E.E. (Ed.), Venomous Animals and their Venoms. Vol.2. Venomous Vertebrates. Academic Press, New York.

[23] Soerensen B., Barros A.R., Zezza Neto L.Z, Oliveira A.M., Santos R.V., Messias C.V., Silva A.R.C., Capossoli E.A., Cavalcante N.B.C., Vellucci S.C.C., Repetti E., Santos P.C.G., Pacchini C.E. & Alves Junior M. 1995. Aspecto clínico e laboratorial do envenenamento botrópico e crotálico em bovinos. Unimar Ciências, Marília, 4(2):28-33.

[24] Sousa M.G., Tokarnia C.H., Brito M.F., Reis A.B., Oliveira C.M., Freitas N.F., Oliveira C.H. & Barbosa J.D. 2011. Aspectos clínico-patológicos do envenenamento Botrópico experimental em equinos. Pesq. Vet. Bras. 31(9):773-780. <https://dx.doi.org/10.1590/S0100-736X2011000900009>
» https://doi.org/10.1590/S0100-736X2011000900009

[25] Takahira R. 1996. Alterações hemáticas e bioquímicas de cães no envenenamento experimental por Bothrops jararaca (Wiedi, 1824) e Bothrops newiedii (Wangler, 1824). Dissertação (Mestrado), Universidade Estadual Paulista, Botucatu, SP.

[26] Thrall A.M., Weiser G., Allison R.W. & Campbell T.W. 2014. Hematologia e Bioquímica Clínica Veterinária. 2nd ed. Roca, São Paulo. 688p.

[27] Tolentino L.H.O., Tolentino M.L.D.L., Assis D.M., Firmino M.O., Benvenutti M.E.M., Miranda Neto E.G., Dantas A.F.M. & Vaz A.F.M. 2019. Caracterização clínica, laboratorial e patológica de equino naturalmente acometido por acidente botrópico. Pubvet 13(4):1-8. <https://dx.doi.org/10.31533/pubvet.v13n4a309.1-8>
» https://doi.org/10.31533/pubvet.v13n4a309.1-8

[28] WHO 2007. Rabies and Envenomings: a neglected public health issue. World Health Organization, Geneva. 32p.

Serum biochemical index	Baseline	After 1st cycle of immunizations	After 2nd cycle of immunizations	After 3rd cycle of immunizations	Total
Urea (mg/dL)	34.0a ± 3.4	26.6b ± 2.7	30.0ab ± 4.2	30.0ab ± 1.2	28.8 ± 4.2
Creatinine (mg/dL)	1.3 ± 0.2	1.3 ± 0.3	1.3 ± 0.4	1.3 ± 0.3	1.3 ± 0.3
Total protein (g/dL)	7.8b ± 0.5	9.9a ± 0.4	10.1a ± 0.5	10.4a ± 1.0	9.0 ± 1.3
Albumin (g/dL)	2.5 ± 0.2	2.2 ± 0.1	2.4 ± 0.2	2.4 ± 0.4	2.4 ± 0.3
AST (IU/L)	140.4b ± 18.4	267.4a ± 34.5	326.4a ± 51.6	330.6a ± 49.9	254.7 ± 78.9
ALT (IU/L)	12.0a ± 0.7	6.6b ± 2.3	6.0b ± 1.9	8.0b ± 1.0	9.8 ± 5.1
GLDH (UI/L)	5.3b ± 1.8	7.2a ± 3.4	4.2ab ± 1.7	2.5ab ± 0.5	4.6 ± 2.1
GGT (IU/L)	4.6c ± 1.9	13.4b ± 4.4	21.6a ± 9.6	17.8ab ± 3.6	11.4 ± 7.4
FA (IU/L)	139.0b ± 20.8	252.0a ± 71.8	250.6a ± 82.5	266.6a ± 77.5	219.5 ± 78.3

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