Your search keyword '"B. Dungu"' showing total 72 results

1. Study on the efficacy and safety of different antigens and oil formulations of infectious coryza vaccines containing an NAD-independent strain of Avibacterium paragallinarum

Author

B. Dungu, B. Brett, R. MacDonald, S. Deville, L. Dupuis, J. Theron, and R.R. Bragg

Subjects

Veterinary medicine, SF600-1100

Abstract

The present study was designed to assess and compare three different formulations of the new Onderstepoort infectious coryza (IC) quadrivalent vaccine, which contain an NAD-independent strain of Avibacterium paragallinarum (previously known as Haemophilus paragallinarum), and a commercial IC vaccine, not containing an NAD-independent strain, for their safety and ability to protect chickens of varying ages against virulent challenges with four different serovars of A. paragallinarum, including the NAD-independent strain of the C-3 serovar. Four groups of 140 chickens each were vaccinated at the age of 17 weeks and revaccinated at the age of 19 weeks with each of the four vaccine formulations. A similar sized group of non-vaccinated chickens was used as control. Two rounds of challenge were conducted: a group of chicken in each vaccination group was challenged between 31 and 35 weeks of age, while another group was challenged between 51 and 55 weeks of age. The ''in-contact'' challenge model was used in this experiment. For each vaccination group, the four challenge strains representing four local serovars were used in each challenge round. The efficacy of the vaccines was compared based on overall protection levels obtained and the duration of protection. The safety of the different vaccines was determined by the severity of post-vaccination reactions. The need for the incorporation of the NAD-independent strain in the vaccine was evidenced by the low protection level against NAD-independent challenge recorded in the group of birds vaccinated with the commercial vaccine. The results obtained confirmed not only the variation in virulence of different South African serovars, with serovar C-3 being the most virulent and serovar B having almost no virulence but also the age related increase in susceptibility. The importance of a suitable formulation of the vaccine is discussed.

Published

2009

2. Evaluation of different adjuvants for foot-and-mouth disease vaccine containing all the SAT serotypes

Author

M. Cloete, B. Dungu, L.I. Van Staden, N. Ismail-Cassim, and W. Vosloo

Subjects

Veterinary medicine, SF600-1100

Abstract

Foot-and-mouth disease (FMD) is an economically important disease of cloven-hoofed animals that is primarily controlled by vaccination of susceptible animals and movement restrictions for animals and animal-derived products in South Africa. Vaccination using aluminium hydroxide gel-saponin (AS) adjuvanted vaccines containing the South African Territories (SAT) serotypes has been shown to be effective both in ensuring that disease does not spread from the endemic to the free zone and in controlling outbreaks in the free zone. Various vaccine formulations containing antigens derived from the SAT serotypes were tested in cattle that were challenged 1 year later. Both the AS and ISA 206B vaccines adjuvanted with saponin protected cattle against virulent virus challenge. The oilbased ISA 206B-adjuvanted vaccine with and without stimulators was evaluated in a field trial and both elicited antibody responses that lasted for 1 year. Furthermore, the ISA 206 adjuvanted FMD vaccine protected groups of cattle against homologous virus challenge at very low payloads, while pigs vaccinated with an emergency ISA 206B-based FMD vaccine containing the SAT 1 vaccine strains were protected against the heterologous SAT 1 outbreak strain.

Published

2008

3. Discrimination between sheep-associated and wildebeest-associated malignant catarrhal fever virus by means of a single-tube duplex nested PCR

Author

C.W. Bremer, H. Swart, F.A. Doboro, B. Dungu, M. Romito, and G.J. Viljoen

Subjects

Veterinary medicine, SF600-1100

Abstract

A single-tube duplex nested polymerase chain reaction (sdn-PCR) was developed for the detection of and discrimination between ovine herpesvirus-2 (OvHV-2) and alcelaphine herpesvirus-1 (AlHV-1). These viruses respectively cause sheep- and wildebeest-associated malignant catarrhal fever (SAMCF and WA-MCF). In the first step of the sdn-PCR, two primers with high annealing temperatures based on conserved regions of the tegument genes were used for DNA amplification. In the second step, two primer sets based on variable regions of the respective OvHV-2 and AlHV-1 genes and with annealing temperatures > 11 °C below the primers used in the first step, were used. Internal regions of different sizes from amplicons produced in the first step were amplified. This single-tube test obviates the need for two separate assays to detect both viral types, thereby reducing time, labour and cost.

Published

2005

4. The role of vaccine banks in resilience, response and recovery in respect of animal diseases

Author

B Dungu

Subjects

Finance, medicine.medical_specialty, business.industry, Public health, Legislature, General Medicine, Disease, Resilience (organizational), Vaccination, Public–private partnership, Countermeasure, medicine, media_common.cataloged_instance, Animal Science and Zoology, Business, European union, media_common

Abstract

Veterinary vaccine banks, also referred to as vaccine stockpiles or vaccine strategic reserves, play an important role in the response to infectious animal diseases, by assisting control of the disease and resilience in recovering from its effects. Vaccine banks have a part to play in both emergencies and control programmes. The concept of vaccine banks was initially established as a countermeasure to an animal disease emergency or outbreak or the introduction of a new disease. They have increasingly been used to prevent important diseases identified by Veterinary Authorities as requiring a well-planned control programme through vaccination. Vaccine banks can consist of physical or virtual reserves, or the maintenance of production capacity. Physical reserves comprise vaccine antigen or readyto-use vaccines. Virtual reserves include inventory management by vaccine manufacturers. Maintenance of production capacity encompasses management of the vaccine seed material, and the maintenance of knowledge by the manufacturers through continued research into the target vaccines. The establishment, maintenance and implementation of vaccine banks depend on a number of prerequisites, which include a strategy for the physical or virtual vaccine stockpile, a legislative framework, regulatory arrangements, effective supply-chain mechanisms and adequate surveillance systems. Through international solidarity, vaccine banks are available and accessible to countries that do not have their own reserves. The World Organisation for Animal Health and European Union vaccine banks perform this task. Moreover, vaccine banks have facilitated access to important public health vaccines, such as rabies vaccines. These issues are discussed below, as well as potential opportunities for public-private partnerships in different aspects of vaccine banks.

Published

2020

5. Rift Valley fever and the challenges of remaining fully prepared for this periodic emergency

Author

B. Dungu and A. Anyamba

Subjects

Rift, Geography, Applied Mathematics, General Mathematics, medicine, Rift Valley fever, medicine.disease, Humanities

Published

2020

6. Safety and immunogenicity of a live attenuated Rift Valley Fever recombinant arMP-12ΔNSm21/384 vaccine candidate for sheep, goats and calves

Author

Zahra Bamouh, B. Dungu, Douglas M. Watts, Khalid Omari Tadlaoui, Mohammed Jazouli, Daouam S, Z. Boumart, Mehdi Elharrak, and G. Bettinger

Subjects

Rift Valley Fever, 030231 tropical medicine, Virulence, Cattle Diseases, Sheep Diseases, Vaccines, Attenuated, Virus Replication, Virus, 03 medical and health sciences, 0302 clinical medicine, Immunogenicity, Vaccine, Neutralization Tests, Chlorocebus aethiops, medicine, Animals, 030212 general & internal medicine, Rift Valley fever, Vero Cells, Infectivity, Vaccines, Synthetic, Sheep, General Veterinary, General Immunology and Microbiology, biology, Immunogenicity, Goats, Public Health, Environmental and Occupational Health, Antibody titer, Viral Vaccines, medicine.disease, Rift Valley fever virus, Virology, Antibodies, Neutralizing, Titer, Morocco, Infectious Diseases, Immunoglobulin G, biology.protein, Molecular Medicine, Cattle, Antibody

Abstract

Rift Valley fever (RVF) causes serious health and economic losses to the livestock industry as well as a significant cause of human disease. The prevention of RVF in Africa is a global priority, however, available vaccines have only been partially effective. Therefore, the objective of this study was to evaluate the safety and immunogenicity of a live, attenuated recombinant RVFV arMP-12ΔNSm21/384 nucleotide deletion vaccine candidate in domestic ruminants. Evaluation involved testing to determine the infectivity titer of the vaccine virus in Vero cells for industrial scale up vaccine production. Safety experiments were conducted to determine the potential of the vaccine virus to revert to virulence by serial passages in sheep, the possibility of virus spread from vaccinated sheep and calves to unvaccinated animals, and the potential health effects of administering overdoses of the vaccine to sheep, goats and calves. The immunogenicity of 3 doses of 104, 105 and 106 Tissue Culture Infectious Doses50% (TCID50) of the vaccine was assessed in 3 groups of 10 sheep and 3 groups of 10 goats, and doses of 105, 106 and 107 TCID50 was evaluated in 3 groups of 10 calves subcutaenous vaccintation. The results showed that the infectivity titer of the vaccine virus was 108.4 TCID50/ml, that the vaccine did not spread from vaccinated to un-vaccinated animals, there was no evidence of reversion to virulence in sheep and the vaccine overdoses did not cause any adverse effects. The immunogenicity among sheep, goats and calves indicated that doses of 104-106 TCID50 elicited detectable antibody by day 7 post-vaccination (PV) with antibody titers ranging from 0.6 log to 2.1 log on day 14 PV with sustained titers through day 28 PV. Overall, these findings indicated that the RVFV arMP-12ΔNSm21/384 vaccine is a promising candidate for the prevention of RVF among domestic ruminants.

Published

2018

7. Development of a safer vaccine against African horse sickness

Author

B. Dungu

Subjects

biology, business.industry, Applied Mathematics, General Mathematics, SAFER, Medicine, African horse sickness, business, biology.organism_classification, Humanities

Published

2019

8. Animal trypanosomosis: making quality control of trypanocidal drugs possible

Author

R C Mattioli, F Araya, B Dungu, A Cannavan, J J Sasanya, Oliver B. Sutcliffe, F van Gool, S Münstermann, and Graham G. Skellern

Subjects

business.industry, media_common.quotation_subject, General Medicine, medicine.disease, Counterfeit, Biotechnology, chemistry.chemical_compound, chemistry, Agriculture, Environmental health, Agency (sociology), medicine, Animal Science and Zoology, Livestock, Quality (business), Isometamidium chloride, business, Trypanosomiasis, Quality assurance, media_common

Abstract

African animal trypanosomosis is arguably the most important animal disease impairing livestock agricultural development in sub-Saharan Africa. In addition to vector control, the use oftrypanocidal drugs is important in controlling the impact of the disease on animal health and production in most sub-Saharan countries. However, there are no internationally agreed standards (pharmacopoeia-type monographs or documented product specifications) for the quality control of these compounds. This means that it is impossible to establish independent quality control and quality assurance standards for these agents. An international alliance between the Food and Agriculture Organization of the United Nations, the International Federation for Animal Health, the Global Alliance for Livestock Veterinary Medicines, the University of Strathclyde and the International Atomic Energy Agency (with critical support from the World Organisation for Animal Health) was established to develop quality control and quality assurance standards for trypanocidal drugs, with the aim of transferring these methodologies to two control laboratories in sub-Saharan Africa that will serve as reference institutions for their respective regions. The work of the international alliance will allow development of control measures against sub-standard or counterfeit trypanocidal drugs for treatment of trypanosome infection. Monographs on diminazene aceturate (synonym: diminazene diaceturate), isometamidium chloride hydrochloride, homidium chloride and bromide salts and their relevant veterinary formulations for these agents are given in the annex to this paper. However, the authors do not recommend use of homidium bromide and chloride, because of their proven mutagenic properties in some animal test models and their suspected carcinogenic properties.

Published

2014

9. Evaluation of different adjuvants for foot-and-mouth disease vaccine containing all the SAT serotypes

Author

L.I. Van Staden, N. Ismail-Cassim, B Dungu, Wilna Vosloo, and M. Cloete

Subjects

Serotype, Veterinary medicine, Swine, Virulence, Cattle Diseases, Sheep Diseases, Aluminum Hydroxide, control strategies, Antibodies, Viral, Virus, South Africa, Antigen, Adjuvants, Immunologic, Medicine, Animals, Serotyping, Adjuvant, Swine Diseases, Sheep, lcsh:Veterinary medicine, General Veterinary, biology, Foot-and-mouth disease, business.industry, Vaccination, Outbreak, pigs, Viral Vaccines, General Medicine, vaccines, Saponins, medicine.disease, Virology, cattle, Foot-and-Mouth Disease Virus, foot-and-mouth disease, Foot-and-Mouth Disease, biology.protein, lcsh:SF600-1100, Cattle, Antibody, Safety, business, Oils

Abstract

Foot-and-mouth disease (FMD) is an economically important disease of cloven-hoofed animals that is primarily controlled by vaccination of susceptible animals and movement restrictions for animals and animal-derived products in South Africa. Vaccination using aluminium hydroxide gel-saponin (AS) adjuvanted vaccines containing the South African Territories (SAT) serotypes has been shown to be effective both in ensuring that disease does not spread from the endemic to the free zone and in controlling outbreaks in the free zone. Various vaccine formulations containing antigens derived from the SAT serotypes were tested in cattle that were challenged 1 year later. Both the AS and ISA 206B vaccines adjuvanted with saponin protected cattle against virulent virus challenge. The oilbased ISA 206B-adjuvanted vaccine with and without stimulators was evaluated in a field trial and both elicited antibody responses that lasted for 1 year. Furthermore, the ISA 206 adjuvanted FMD vaccine protected groups of cattle against homologous virus challenge at very low payloads, while pigs vaccinated with an emergency ISA 206B-based FMD vaccine containing the SAT 1 vaccine strains were protected against the heterologous SAT 1 outbreak strain.

Published

2008

10. Alternative vaccination against equine botulism (BoNT/C)

Author

Christelle Mazuet, Michel R. Popoff, S. Eberle, V. Gerber, E. Schatzmann, Christina Stahl, B. Dungu, Joachim Frey, and Reto Straub

Subjects

Male, Botulinum Toxins, Vaccination schedule, medicine.medical_treatment, Blotting, Western, Immunization, Secondary, Enzyme-Linked Immunosorbent Assay, Serology, Mice, Adjuvants, Immunologic, Neutralization Tests, medicine, Animals, Botulism, Horses, Seroconversion, Immunization Schedule, Vaccines, Synthetic, biology, business.industry, General Medicine, medicine.disease, Antibodies, Bacterial, Virology, Bacterial vaccine, Vaccination, Immunoglobulin G, Bacterial Vaccines, Immunology, biology.protein, Biological Assay, Female, Horse Diseases, Antibody, business, Adjuvant

Abstract

REASON FOR PERFORMING STUDY: In Europe the incidence of botulism in horses has increased in the last decade due to the growing popularity of haylage feeding. Recombinant vaccines are safer and less expensive to produce and are generally better tolerated than toxoids. OBJECTIVES: To investigate whether the recombinant C-terminal half of the heavy chain of the botulinum neurotoxin C (Hc BoNT/C) in combination with an immunstimulatory adjuvant is an appropriate vaccine candidate for horses by testing its efficacy to induce neutralising antibodies and by comparing its immunogenic properties and adverse reactions to a commercial toxoid vaccine. Formation of oedema and local pain reactions were assessed. ELISA and Western blot assay against Hc BoNT/C and testing of neutralising antibody induction in a mouse protection assay were used to evaluate the immune response. RESULTS: With the recombinant vaccine, only minor local swelling with full recovery after 5 days was noted after brisket injections. The toxoid vaccine produced local, painful reactions with longer recovery periods of up to 2 weeks. Horses vaccinated with either vaccine induced neutralising antibodies after the second booster vaccination, while seroconversion on ELISA and Western blot to Hc BoNT/C was apparent after the first recombinant vaccination, and at various time points in the vaccination schedule in horses that received commercial toxoid vaccine. CONCLUSION: The recombinant vaccine showed fewer adverse reactions compared to the only commercially available vaccine but induced similar concentrations of neutralising antibodies. There was no correlation between the serological response to Hc BoNT/C and the neutralising capacity of serum. POTENTIAL RELEVANCE: Recombinant Hc BoNT/C is an appropriate vaccine candidate to stimulate production of neutralising antibodies against botulinum neurotoxin C in horses and creates only minor local reactions at the injection site.

Published

2007

11. La vacunas veterinarias y su utilización en los paises en desarollo

Author

B Dungu, Mark M. Rweyemamu, W Amanfu, G Viljoen, A Diallo, and J. Lubroth

Subjects

Veterinary medicine, Government, Food security, business.industry, media_common.quotation_subject, Developing country, General Medicine, Vaccination, Animal welfare, Medicine, Animal Science and Zoology, Livestock, Quality (business), business, Constraint (mathematics), media_common

Abstract

The burden of infectious diseases in livestock and other animals continues to be a major constraint to sustained agricultural development, food security, and participation of developing and in-transition countries in the economic benefits of international trade in livestock commodities. Targeted measures must be instituted in those countries to reduce the occurrence of infectious diseases. Quality veterinary vaccines used strategically can and should be part of government sanctioned-programmes. Vaccination campaigns must be part of comprehensive disease control programmes, which, in the case of transboundary animal diseases, require a regional approach if they are to be successful. This paper focuses on the salient transboundary animal diseases and examines current vaccine use, promising vaccine research, innovative technologies that can be applied in countries in some important developing regions of the world, and the role of public/private partnerships.

Published

2007

12. Animal trypanosomosis: making quality control of trypanocidal drugs possible

Author

O B, Sutcliffe, G G, Skellern, F, Araya, A, Cannavan, J J, Sasanya, B, Dungu, F, van Gool, S, Münstermann, and R C, Mattioli

Subjects

Internationality, Trypanosomiasis, African, Molecular Structure, Animals, Veterinary Drugs, Trypanocidal Agents, Africa South of the Sahara

Abstract

African animal trypanosomosis is arguably the most important animal disease impairing livestock agricultural development in sub-Saharan Africa. In addition to vector control, the use oftrypanocidal drugs is important in controlling the impact of the disease on animal health and production in most sub-Saharan countries. However, there are no internationally agreed standards (pharmacopoeia-type monographs or documented product specifications) for the quality control of these compounds. This means that it is impossible to establish independent quality control and quality assurance standards for these agents. An international alliance between the Food and Agriculture Organization of the United Nations, the International Federation for Animal Health, the Global Alliance for Livestock Veterinary Medicines, the University of Strathclyde and the International Atomic Energy Agency (with critical support from the World Organisation for Animal Health) was established to develop quality control and quality assurance standards for trypanocidal drugs, with the aim of transferring these methodologies to two control laboratories in sub-Saharan Africa that will serve as reference institutions for their respective regions. The work of the international alliance will allow development of control measures against sub-standard or counterfeit trypanocidal drugs for treatment of trypanosome infection. Monographs on diminazene aceturate (synonym: diminazene diaceturate), isometamidium chloride hydrochloride, homidium chloride and bromide salts and their relevant veterinary formulations for these agents are given in the annex to this paper. However, the authors do not recommend use of homidium bromide and chloride, because of their proven mutagenic properties in some animal test models and their suspected carcinogenic properties.

Published

2015

13. Foot and mouth disease in Mali: the current situation and proposed control strategies

Author

Armanda D.S. Bastos, B Dungu, and Oumou Sangare

Subjects

Veterinary medicine, medicine.medical_specialty, Cattle Diseases, Fmd virus, Mali, Disease Outbreaks, West africa, parasitic diseases, Epidemiology, Animals, Medicine, Socioeconomics, Disease Reservoirs, Foot-and-mouth disease, business.industry, Transmission (medicine), Vaccination, High mortality, Outbreak, General Medicine, medicine.disease, Foot-and-Mouth Disease, Cattle, Animal Science and Zoology, Livestock, business

Abstract

Two main reasons prompted the authors to write this paper. First, outbreaks of foot and mouth disease (FMD) have occurred repeatedly in Mali and neighbouring countries during the last decade. Secondly, there is a pressing need for control strategies, since the first molecular epidemiological studies of FMD virus in West Africa have demonstrated that FMD transmission across national boundaries is common in this region. The authors discuss the FMD outbreaks that occurred during the period of 1980 to 1996, which were reported to the Central Livestock Office in Mali by field veterinarians. The outbreaks in 1980 and 1982 were confined to the regions of Kayes and Gao, respectively. Between 1991 and 1992, outbreaks occurred in Segou, Sikasso and Bamako. In 1996, FMD outbreaks were reported in cattle populations throughout Mali, except in Kidal in the Sahara desert, where temperatures reach 45 degrees C. High mortality was reported in young animals, while morbidity approached 100% in adult cattle.

Published

2004

14. Evaluation of two PCR-based procedures for typing Clostridium perfringens : research communication

Author

H. Fourie, A. Bosman, M.M. Henton, G. Viljoen, and B. Dungu

Subjects

lcsh:Veterinary medicine, General Veterinary, Toxin, General Medicine, Clostridium perfringens, Biology, medicine.disease_cause, Virology, Polymerase Chain Reaction, Microbiology, law.invention, Skin reaction, Clostridium Perfringens, In vivo, law, Multiplex polymerase chain reaction, medicine, Toxin typing, lcsh:SF600-1100, Typing, Toxin Typing, Polymerase chain reaction

Abstract

Two polymerase chain reaction (PCR)-based procedures for typing Clostridium perfringens, which affects most domestic animals, were compared and evaluated for efficiency as substitute to the guinea-pig intradermal test routinely used in our laboratory, namely a multiplex PCR and a protocol based on the individual amplification of gene sequences specific for each toxin. Reference isolates of C. perfringens types A, B, C and D as well as cultures from clinical specimens were tested. The sensitivity and specificity of the PCR was confirmed on reference isolates. There was similarity in results on 43 of the 46 samples typed by all 3 methods. Clear results were obtained by PCR on 5 clinical samples that showed either equivocal or weak skin reactions in guinea-pigs. The multiplex PCR protocol, in combination with the evaluation of bacterial growth, is a better alternative to in vivo toxin typing, since C. perfringens can only be incriminated as cause of a disease when it is present in large numbers in the intestine.

Published

2000

15. Vaccination for the control of Rift Valley fever in enzootic and epizootic situations

Author

B, Dungu, M, Donadeu, and M, Bouloy

Subjects

Rift Valley Fever, Vaccination, Animals, Humans, Viral Vaccines, Global Health, Immunization Schedule, Disease Outbreaks

Abstract

Vaccination continues to be the most effective way to control Rift Valley fever (RVF), a zoonotic insect-borne viral disease of livestock. The irregular, cyclical and persistent nature of RVF in its occurrence in enzootic situations suggests that the vaccination strategy to be considered for these regions should be different from what is envisaged for free from risk regions. Currently available RVF vaccines have been extensively used for the control of the disease. However, these vaccines have shortcomings that have encouraged many research groups to develop new vaccine candidates that would address a large number of the current challenges, and be suitable for use both in disease-free regions and in different contingency and emergency preparedness strategies. The characteristics of different RVF vaccines and vaccination strategies are discussed in this report.

Published

2013

16. The use of vaccination in the control of bluetongue in southern Africa

Author

B, Dungu, T, Gerdes, and T, Smit

Abstract

The eradication of bluetongue virus (BTV) from endemic regions of Africa is virtually impossible due to the role played by widely distributed Culicoides spp. midge vectors and the ubiquitous distribution of vertebrate reservoir species. In endemic areas, attempts can only be made to limit the occurrence of bluetongue (BT) disease and its economic impact through vaccination. Despite several potential problems (teratogenicity, risk of reassortment, and reversion to virulence of the attenuated viral strains), the current live-attenuated vaccine, produced by Onderstepoort Biological Products (OBP), South Africa, has been used for decades in enzootic regions, and has been shown to provide a safe and efficacious means to control the disease in regions of southern Africa, as well as other areas of the world.

Published

2010

17. Study on the efficacy and safety of different antigens and oil formulations of infectious coryza vaccines containing an NAD-independent strain of Avibacterium paragallinarum

Author

Robert R. Bragg, S. Deville, Jacques Theron, Raynard Macdonald, L. Dupuis, B. Brett, and B. Dungu

Subjects

Serotype, Haemophilus Infections, Rhinovirus, Avibacterium paragallinarum, Virulence, Biology, coryza vaccine, Virus, Random Allocation, Antigen, Animals, C-3 serovar, Poultry Diseases, lcsh:Veterinary medicine, Picornaviridae Infections, Haemophilus paragallinarum, General Veterinary, NAD-independent strain, Viral Vaccine, Vaccination, Outbreak, Viral Vaccines, General Medicine, NAD, Virology, Bacterial vaccine, Treatment Outcome, Bacterial Vaccines, chickens, lcsh:SF600-1100, Chickens

Abstract

The present study was designed to assess and compare three different formulations of the new Onderstepoort infectious coryza (IC) quadrivalent vaccine, which contain an NAD-independent strain of Avibacterium paragallinarum (previously known as Haemophilus paragallinarum), and a commercial IC vaccine, not containing an NAD-independent strain, for their safety and ability to protect chickens of varying ages against virulent challenges with four different serovars of A. paragallinarum, including the NAD-independent strain of the C-3 serovar. Four groups of 140 chickens each were vaccinated at the age of 17 weeks and revaccinated at the age of 19 weeks with each of the four vaccine formulations. A similar sized group of non-vaccinated chickens was used as control. Two rounds of challenge were conducted: a group of chicken in each vaccination group was challenged between 31 and 35 weeks of age, while another group was challenged between 51 and 55 weeks of age. The ''in-contact'' challenge model was used in this experiment. For each vaccination group, the four challenge strains representing four local serovars were used in each challenge round. The efficacy of the vaccines was compared based on overall protection levels obtained and the duration of protection. The safety of the different vaccines was determined by the severity of post-vaccination reactions. The need for the incorporation of the NAD-independent strain in the vaccine was evidenced by the low protection level against NAD-independent challenge recorded in the group of birds vaccinated with the commercial vaccine. The results obtained confirmed not only the variation in virulence of different South African serovars, with serovar C-3 being the most virulent and serovar B having almost no virulence but also the age related increase in susceptibility. The importance of a suitable formulation of the vaccine is discussed.

Published

2009

18. Veterinary vaccines and their use in developing countries

Author

J, Lubroth, M M, Rweyemamu, G, Viljoen, A, Diallo, B, Dungu, and W, Amanfu

Subjects

International Cooperation, Communicable Disease Control, Vaccination, Commerce, Animals, Humans, Animal Welfare, Developing Countries, Animal Diseases, Food Supply

Abstract

The burden of infectious diseases in livestock and other animals continues to be a major constraint to sustained agricultural development, food security, and participation of developing and in-transition countries in the economic benefits of international trade in livestock commodities. Targeted measures must be instituted in those countries to reduce the occurrence of infectious diseases. Quality veterinary vaccines used strategically can and should be part of government sanctioned-programmes. Vaccination campaigns must be part of comprehensive disease control programmes, which, in the case of transboundary animal diseases, require a regional approach if they are to be successful. This paper focuses on the salient transboundary animal diseases and examines current vaccine use, promising vaccine research, innovative technologies that can be applied in countries in some important developing regions of the world, and the role of public/private partnerships.

Published

2007

19. Discrimination between sheep-associated and wildebeest-associated malignant catarrhal fever virus by means of a single-tube duplex nested PCR

Author

Gerrit J. Viljoen, F.A. Doboro, C.W. Bremer, H. Swart, B. Dungu, and M. Romito

Subjects

viruses, Molecular Sequence Data, Virulence, Sheep Diseases, Biology, Polymerase Chain Reaction, Virus, Animals, Gene, Herpesviridae, DNA Primers, lcsh:Veterinary medicine, Sheep, General Veterinary, Base Sequence, Temperature, General Medicine, Viral tegument, Amplicon, Virology, Molecular biology, Antelopes, Duplex (building), Malignant Catarrh, DNA, Viral, lcsh:SF600-1100, Primer (molecular biology), Nested polymerase chain reaction, Nucleic Acid Amplification Techniques, Sequence Alignment

Abstract

BREMER, C.W., SWART, H., DOBORO, F.A., DUNGU, B., ROMITO, M. & VILJOEN, G.J. 2005. Discrimination between sheep-associated and wildebeest-associated malignant catarrhal fever virus by means of a single-tube duplex nested PCR. Onderstepoort Journal of Veterinary Research, 72:285– 291 A single-tube duplex nested polymerase chain reaction (sdn-PCR) was developed for the detection of and discrimination between ovine herpesvirus-2 (OvHV-2) and alcelaphine herpesvirus-1 (AlHV-1). These viruses respectively cause sheep- and wildebeest-associated malignant catarrhal fever (SAMCF and WA-MCF). In the first step of the sdn-PCR, two primers with high annealing temperatures based on conserved regions of the tegument genes were used for DNA amplification. In the second step, two primer sets based on variable regions of the respective OvHV-2 and AlHV-1 genes and with annealing temperatures > 11 °C below the primers used in the first step, were used. Internal regions of different sizes from amplicons produced in the first step were amplified. This single-tube test obviates the need for two separate assays to detect both viral types, thereby reducing time, labour and cost.

Published

2006

20. Vaccination in the control of bluetongue in endemic regions: the South African experience

Author

B, Dungu, C, Potgieter, B, Von Teichman, and T, Smit

Subjects

South Africa, Sheep, Cost-Benefit Analysis, Vaccination, Animals, Animals, Wild, Viral Vaccines, Bluetongue, Bluetongue virus, Phylogeny, Disease Reservoirs, Insect Vectors

Abstract

The eradication of bluetongue virus (BTV) from endemic regions of Africa is virtually impossible due to the role played by the widely distributed Culicoides spp. of midge vectors and the ubiquitous distribution of reservoir species. In endemic areas attempts can only be made to limit the occurrence of bluetongue (BT) disease and its economic impact through vaccination. Despite several potential problems (teratogenicity, risk of reassortment and reversion to virulence of the attenuated viral strains), epidemiological and recent molecular data support the fact that the live attenuated vaccine that has been used for decades in enzootic regions, provides a safe and efficacious means to control the disease in regions of southern Africa, as well as other areas of the world.

Published

2005

21. Foot-and-mouth disease control using vaccination: South African experience

Author

G K, Brückner, W, Vosloo, M, Cloete, B, Dungu, and B J A, Du Plessis

Subjects

South Africa, Sheep, Buffaloes, Animals, Domestic, Foot-and-Mouth Disease, Goats, Communicable Disease Control, Vaccination, Animals, Animals, Wild, Cattle, Antibodies, Viral, Disease Outbreaks

Abstract

South Africa has zoned status from the Office International des Epizooties (OIE) with the largest part of the country being foot-and-mouth disease (FMD)-free without vaccination. Outbreaks in this zone are handled differently from outbreaks in the control zones, which do not affect the export status of the country. However, the different socio-economic groupings need to be considered when reaching control decisions and in this regard, the country has been challenged with unique foot-and-mouth disease (FMD) control options. Vaccination has been shown to be effective both in ensuring that disease does not spread from the endemic to the free zone, as well as controlling outbreaks in the free zone. New adjuvants that claim to illicit longer lasting immunity have been tested with antigens derived from the SAT serotypes and animals were challenged one year post vaccination to determine the level of protection. However, even with vaccines that provide immunity for more than a year, an annual vaccination campaign will most probably not be acceptable in the buffer zone where calving occurs throughout the year.

Published

2005

22. Suitability of currently available vaccines for controlling the major transboundary diseases that afflict sub-Saharan Africa

Author

G, Thomson, B, Dungu, K, Tounkara, W, Vosloo, A, Bastos, and K, Bidjeh

Subjects

Rinderpest, Swine, Animals, Domestic, Foot-and-Mouth Disease, Vaccination, Animals, Cattle Diseases, Cattle, Viral Vaccines, African Swine Fever, Pleuropneumonia, Contagious, Africa South of the Sahara, Animal Diseases

Published

2003

23. Single-tube nested PCR for detection of the sheep-associated agent of MCF

Author

B, Dungu, A M, Bosman, C, Kachelhoffer, and G J, Viljoen

Subjects

Sheep, Malignant Catarrh, DNA, Viral, Animals, Sheep Diseases, Cattle, Polymerase Chain Reaction, Sensitivity and Specificity, Herpesviridae

Published

2003

24. Validation of an indirect enzyme-linked immunosorbent assay for the detection of antibody against Brucella abortus in cattle sera using an automated ELISA workstation

Author

J T, Paweska, A D, Potts, H J, Harris, S J, Smith, G J, Viljoen, B, Dungu, O L, Brett, M, Bubb, and L, Prozesky

Subjects

Quality Control, Rose Bengal, Complement Fixation Tests, Brucella abortus, Reproducibility of Results, Enzyme-Linked Immunosorbent Assay, Antibodies, Bacterial, Sensitivity and Specificity, Brucellosis, Bovine, Reference Values, Agglutination Tests, Animals, Cattle, Fluorescent Dyes

Abstract

An automated indirect enzyme-linked immunosorbent assay (I-ELISA) for the serological diagnosis of bovine brucellosis was developed and validated in-house. A total of 4,803 cattle sera from South Africa (n = 3,643), Canada (n = 652), Germany (n = 240), France (n = 73) and the USA (n = 195) was used. The South African panel of sera represented 834 sera known to be positive by the Rose Bengal test (RBT), serum agglutination test (SAT) and complement fixation test (CFT), 2709 sera that were negative by CFT, and 100 sera from animals vaccinated with a standard dose of Brucella abortus strain 19. Overseas sera were obtained from reference non-vaccinated brucella-free cattle (n = 834), naturally infected (n = 72), experimentally infected (n = 71), and vaccinated animals (n = 83). Also 100 sera collected from cattle in Canada and known to be positive by competitive ELISA (C-ELISA) were used. The intermediate ranges ("borderline" range for the interpretation of test results) were derived from two-graph receiver operating characteristics analysis. The lowest values of the misclassification cost-term analysis obtained from testing overseas panels, covered lower I-ELISA cut-off PP values (0.02-3.0) than those from local panels (1.5-5.0). The relatively low cut-off PP values selected for I-ELISA were due to the fact that the positive control used represents a very strong standard compared to other reference positive sera. The greater overlap found between negative and positive cattle sera from South Africa than that between reference overseas panels was probably due to the different criteria used in classifying these panels as negative (sera from true non-diseased/non-infected animals) or positive (sera from true diseased/infected animals). The diagnostic sensitivity of the I-ELISA (at the optimum cut-off value) was 100% and of the CFT 83.3%. The diagnostic specificity of I-ELISA was 99.8% and of the CFT 100%. Estimate of Youden's index was higher for the I-ELISA (0.998) than that for the CFT (0.833). Analysis of distribution of PP values in sera from vaccinated and naturally infected cattle shows that in vaccinated animals all readings were below 31 PP where in infected ones these values represented 43%. Therefore, it appears that I-ELISA could be of use in identifying some naturally infected animals (with values31 PP), but more sera from reference vaccinated and infected animals need to be tested to further substantiate this statistically. Of 834 sera positive by RBT, SAT and CFT, 825 (98.9%) were positive in the I-ELISA. Compared to C-ELISA the relative diagnostic sensitivity of the I-ELISA was 94% and of the CFT 88% when testing 100 Canadian cattle sera. Of 258 South African cattle sera, of which 183 (70.9 %) were positive by the I-ELISA and 148 (57.4 %) by the CFT, 197 (76.4%) were positive by C-ELISA when re-tested in Canada. One has to stress, however, that Canadian C-ELISA has not been optimised locally. Thus, the C-ELISA was probably not used at the best diagnostic threshold for testing South African cattle sera. This study shows that the I-ELISA performed on an automated ELISA workstation provides a rapid, simple, highly sensitive and specific diagnostic system for large-scale detection of antibodies against B. abortus. Based on the diagnostic accuracy of this assay reported here, the authors suggest that it could replace not only the currently used confirmatory CFT test, but also the two in-use screening tests, namely the RBT and SAT.

Published

2002

25. Evaluation of two PCR-based procedures for typing Clostridium perfringens

Author

B, Dungu, M M, Henton, A, Bosman, H, Fourie, and G, Viljoen

Subjects

Electrophoresis, Agar Gel, Enterotoxins, Genotype, Clostridium perfringens, Guinea Pigs, Animals, Intradermal Tests, Polymerase Chain Reaction, Bacterial Typing Techniques

Abstract

Two polymerase chain reaction (PCR)-based procedures for typing Clostridium, perfringens, which affects most domestic animals, were compared and evaluated for efficiency as substitute to the guinea-pig intradermal test routinely used in our laboratory, namely a multiplex PCR and a protocol based on the individual amplification of gene sequences specific for each toxin. Reference isolates of C. perfringens types A, B, C and D as well as cultures from clinical specimens were tested. The sensitivity and specificity of the PCR was confirmed on reference isolates. There was similarity in results on 43 of the 46 samples typed by all 3 methods. Clear results were obtained by PCR on 5 clinical samples that showed either equivocal or weak skin reactions in guinea-pigs. The multiplex PCR protocol, in combination with the evaluation of bacterial growth, is a better alternative to in vivo toxin typing, since C. perfringens can only be incriminated as cause of a disease when it is present in large numbers in the intestine.

Published

2000

26. The effect of a natural maedi-visna virus infection on the productivity of South African sheep

Author

B, Dungu, J, Vorster, G F, Bath, and D W, Verwoerd

Subjects

Male, Sheep, Visna-maedi virus, Pneumonia, Progressive Interstitial, of Sheep, Mastitis, Antibodies, Viral, Cohort Studies, South Africa, Mammary Glands, Animal, Milk, Animals, Female, Lymphocytes, Growth Disorders

Abstract

A cohort study was conducted in order to measure the effect of the chronic indurative lymphocytic mastitis caused by the South African strain of maedi visna virus (MVV) on the pre-weaning growth of lambs born either of naturally infected or uninfected ewes kept under similar conditions. Fifty naturally infected ewes as well as another 40 from a maedi-visna-free source to be used as control animals, were purchased and kept in separate flocks which were managed in a similar way. All the ewes were of the same breed and 3-4 years old. During the adaptation period, and through the mating, pregnancy and lactation periods they were periodically monitored for the presence of MVV serum antibodies. The lambs were weighed at birth and thereafter every 2 weeks until the age of 90 days, when they were weaned. The ewes were then slaughtered, and their udders examined histologically and the number of lymphocytic follicles were counted and assessed. Although the calculated values indicated a correlation between the number of follicles in the udder and the reduction in the growth rate of the lambs, this was not statistically significant. Similarly, despite higher counts of lymphoid follicles in the udders of sero-positive ewes as compared to those that were sero-negative and the lower ewe productivity indexes in infected ewes, no statistically significant differences were found in the indexes of ewes in different follicle categories.

Published

2000

27. Detection of Maedi-Visna virus antibodies using a single fusion transmembrane-core p25 recombinant protein ELISA and a modified receiver-operating characteristic analysis to determine cut-off values

Author

R. Williams, J.D. Conradie, J. Vorster, B. Dungu, C.H. Boshoff, D.F. York, and D. W. Verwoerd

Subjects

Visna-maedi virus, Visna virus, Recombinant Fusion Proteins, Gene Products, gag, Enzyme-Linked Immunosorbent Assay, Antibodies, Viral, Virus, law.invention, Visna, Antigen, law, Virology, Escherichia coli, Animals, Cloning, Molecular, Antigens, Viral, Expression vector, Sheep, biology, biology.organism_classification, Fusion protein, Molecular biology, female genital diseases and pregnancy complications, eye diseases, biology.protein, Recombinant DNA, Antibody

Abstract

The core p25 and transmembrane (TM) genes of Maedi-Visna virus (MVV) were cloned individually into the pGEX-2T expression vector. Both proteins were expressed as a combined fusion protein in frame with glutathione S-transferase (GST). The purified recombinant antigens (GST-TM and GST-TM-p25) were used to develop a MVV ELISA. A preliminary assessment of the diagnostic potential of the recombinant antigens (GST-TM and GST-TM-p25) was made by testing the antigens against 46 seropositive and 46 seronegative sheep and comparing the results with a commercial p25 ELISA kit. A two-graph receiver operating characteristic (TG-ROC) analysis program was used to interpret the data. The GST-TM-p25 ELISA was more sensitive than the commercial assay which is based on the p25 antigen alone and more specific than the GST-TM ELISA.

Published

1997

28. A perspective on Maedi-Visna in South Africa

Author

J H, Vorster, B, Dungu, L C, Marais, D F, York, R, Williams, and C H, Boshoff

Subjects

South Africa, Sheep, Visna-maedi virus, Pneumonia, Progressive Interstitial, of Sheep, Animals

Published

1996

29. The panzootic spread of highly pathogenic avian influenza H5N1 sublineage 2.3.4.4b: a critical appraisal of One Health preparedness and prevention.

Author

Koopmans MPG, Barton Behravesh C, Cunningham AA, Adisasmito WB, Almuhairi S, Bilivogui P, Bukachi SA, Casas N, Cediel Becerra N, Charron DF, Chaudhary A, Ciacci Zanella JR, Dar O, Debnath N, Dungu B, Farag E, Gao GF, Khaitsa M, Machalaba C, Mackenzie JS, Markotter W, Mettenleiter TC, Morand S, Smolenskiy V, Zhou L, and Hayman DTS

Abstract

Changes in the epidemiology and ecology of H5N1 highly pathogenic avian influenza are devastating wild bird and poultry populations, farms and communities, and wild mammals worldwide. Having originated in farmed poultry, H5N1 viruses are now spread globally by wild birds, with transmission to many mammal and avian species, resulting in 2024 in transmission among dairy cattle with associated human cases. These ecological changes pose challenges to mitigating the impacts of H5N1 highly pathogenic avian influenza on wildlife, ecosystems, domestic animals, food security, and humans. H5N1 highly pathogenic avian influenza highlights the need for One Health approaches to pandemic prevention and preparedness, emphasising multisectoral collaborations among animal, environmental, and public health sectors. Action is needed to reduce future pandemic risks by preventing transmission of highly pathogenic avian influenza among domestic and wild animals and people, focusing on upstream drivers of outbreaks, and ensuring rapid responses and risk assessments for zoonotic outbreaks. Political commitment and sustainable funding are crucial to implementing and maintaining prevention programmes, surveillance, and outbreak responses., Competing Interests: Declaration of interests All authors declare no competing interests., (Copyright © 2024 Elsevier Ltd. All rights reserved, including those for text and data mining, AI training, and similar technologies.)

Published

2024

30. Correction: The One Health High-Level Expert Panel (OHHLEP).

Author

Mettenleiter TC, Markotter W, Charron DF, Adisasmito WB, Almuhairi S, Behravesh CB, Bilivogui P, Bukachi SA, Casas N, Becerra NC, Chaudhary A, Ciacci Zanella JR, Cunningham AA, Dar O, Debnath N, Dungu B, Farag E, Gao GF, Hayman DTS, Khaitsa M, Koopmans MPG, Machalaba C, Mackenzie JS, Morand S, Smolenskiy V, and Zhou L

Published

2024

31. The One Health High-Level Expert Panel (OHHLEP).

Author

Mettenleiter TC, Markotter W, Charron DF, Adisasmito WB, Almuhairi S, Behravesh CB, Bilivogui P, Bukachi SA, Casas N, Becerra NC, Chaudhary A, Zanella JRC, Cunningham AA, Dar O, Debnath N, Dungu B, Farag E, Gao GF, Hayman DTS, Khaitsa M, Koopmans MPG, Machalaba C, Mackenzie JS, Morand S, Smolenskiy V, and Zhou L

Published

2023

32. Prevention of zoonotic spillover: From relying on response to reducing the risk at source.

Author

Markotter W, Mettenleiter TC, Adisasmito WB, Almuhairi S, Barton Behravesh C, Bilivogui P, Bukachi SA, Casas N, Cediel Becerra N, Charron DF, Chaudhary A, Ciacci Zanella JR, Cunningham AA, Dar O, Debnath N, Dungu B, Farag E, Gao GF, Hayman DTS, Khaitsa M, Koopmans MPG, Machalaba C, Mackenzie JS, Morand S, Smolenskiy V, and Zhou L

Subjects

Animals, Humans, Zoonoses epidemiology, Zoonoses prevention & control, Animals, Wild

Abstract

Competing Interests: The authors have declared that no competing interests exist.

Published

2023

33. Developing One Health surveillance systems.

Author

Hayman DTS, Adisasmito WB, Almuhairi S, Behravesh CB, Bilivogui P, Bukachi SA, Casas N, Becerra NC, Charron DF, Chaudhary A, Ciacci Zanella JR, Cunningham AA, Dar O, Debnath N, Dungu B, Farag E, Gao GF, Khaitsa M, Machalaba C, Mackenzie JS, Markotter W, Mettenleiter TC, Morand S, Smolenskiy V, Zhou L, and Koopmans M

Abstract

The health of humans, domestic and wild animals, plants, and the environment are inter-dependent. Global anthropogenic change is a key driver of disease emergence and spread and leads to biodiversity loss and ecosystem function degradation, which are themselves drivers of disease emergence. Pathogen spill-over events and subsequent disease outbreaks, including pandemics, in humans, animals and plants may arise when factors driving disease emergence and spread converge. One Health is an integrated approach that aims to sustainably balance and optimize human, animal and ecosystem health. Conventional disease surveillance has been siloed by sectors, with separate systems addressing the health of humans, domestic animals, cultivated plants, wildlife and the environment. One Health surveillance should include integrated surveillance for known and unknown pathogens, but combined with this more traditional disease-based surveillance, it also must include surveillance of drivers of disease emergence to improve prevention and mitigation of spill-over events. Here, we outline such an approach, including the characteristics and components required to overcome barriers and to optimize an integrated One Health surveillance system., Competing Interests: The authors declare no-conflict of interest., (© 2023 The Authors.)

Published

2023

34. One Health: A new definition for a sustainable and healthy future.

Author

Adisasmito WB, Almuhairi S, Behravesh CB, Bilivogui P, Bukachi SA, Casas N, Cediel Becerra N, Charron DF, Chaudhary A, Ciacci Zanella JR, Cunningham AA, Dar O, Debnath N, Dungu B, Farag E, Gao GF, Hayman DTS, Khaitsa M, Koopmans MPG, Machalaba C, Mackenzie JS, Markotter W, Mettenleiter TC, Morand S, Smolenskiy V, and Zhou L

Subjects

Forecasting, One Health

Abstract

Competing Interests: The authors have declared that no competing interests exist.

Published

2022

35. Field survey of major infectious and reproductive diseases responsible for mortality and productivity losses of ruminants amongst Nigerian Fulani pastoralists.

Author

Bolajoko MB, Van Gool F, Peters AR, Suarez Martinez J, Vance CJ, and Dungu B

Abstract

Background: Animal disease constitutes a major hurdle to improved livelihoods in rural Nigeria through the challenges of loss of productivity, livestock morbidity and mortality including reproductive losses. In order to design and implement impactful interventions, baseline data on the causes of such losses are needed. Therefore, the objective of the present study was to carry out targeted field surveys, including interviews with ruminant farmers, veterinary professionals and other stakeholders in livestock farming to establish the main causes of disease and mortality including abortions in cattle and small ruminants (SR). Methods: Northern Nigeria was selected because the majority of the nation's ruminants belong to pastoralists who are primarily resident in this region. Seven states; Bauchi, Kaduna, Kano, Nasarawa, Niger, Sokoto and Zamfara states were surveyed. The responses were collated and a comprehensive descriptive analysis was carried out. Results: Average cattle herd sizes ranged from 28 in Zamfara to 103 in Nasarawa; and from 27 in Kano to 128 in Sokoto for SR. In cattle, Trypanosomosis (with 4.27% mortality rate), foot and mouth disease (3.81%), nutritional insufficiency (1.93%) and contagious bovine pleuropneumonia (CBPP; 1.44%) were the top four diseases/health problems that resulted in the highest mortality due to diseases within each state surveyed. For SR, trypanosomosis (with 6.85% mortality rate), Peste des Petits Ruminants (4.99%), orf (3.06%), foot rot (2.97%) and foot and mouth disease (2.94%) were the most important diseases responsible for the highest number of mortalities and culling for disease. Conclusions: The study revealed that there are significant losses via mortalities due to the occurrence of disease amongst the ruminant populations countrywide, as evidenced by the high overall mortality rates of both cattle (15.3%) and small ruminants (30.9%) from various diseases. Also, reproductive losses of 8.7% and 16.6% in cattle and SR, respectively, were recorded amongst the farmers involved., Competing Interests: No competing interests were disclosed., (Copyright: © 2020 Bolajoko MB et al.)

Published

2020

36. The role of vaccine banks in resilience, response and recovery in respect of animal diseases.

Author

Dungu B

Subjects

Animals, Disease Outbreaks, Global Health, Vaccination veterinary, Animal Diseases prevention & control, Rabies Vaccines

Abstract

Veterinary vaccine banks, also referred to as vaccine stockpiles or vaccine strategic reserves, play an important role in the response to infectious animal diseases, by assisting control of the disease and resilience in recovering from its effects. Vaccine banks have a part to play in both emergencies and control programmes. The concept of vaccine banks was initially established as a countermeasure to an animal disease emergency or outbreak or the introduction of a new disease. They have increasingly been used to prevent important diseases identified by Veterinary Authorities as requiring a well-planned control programme through vaccination. Vaccine banks can consist of physical or virtual reserves, or the maintenance of production capacity. Physical reserves comprise vaccine antigen or readyto-use vaccines. Virtual reserves include inventory management by vaccine manufacturers. Maintenance of production capacity encompasses management of the vaccine seed material, and the maintenance of knowledge by the manufacturers through continued research into the target vaccines. The establishment, maintenance and implementation of vaccine banks depend on a number of prerequisites, which include a strategy for the physical or virtual vaccine stockpile, a legislative framework, regulatory arrangements, effective supply-chain mechanisms and adequate surveillance systems. Through international solidarity, vaccine banks are available and accessible to countries that do not have their own reserves. The World Organisation for Animal Health and European Union vaccine banks perform this task. Moreover, vaccine banks have facilitated access to important public health vaccines, such as rabies vaccines. These issues are discussed below, as well as potential opportunities for public-private partnerships in different aspects of vaccine banks.

Published

2020

37. Safety and immunogenicity of a live attenuated Rift Valley Fever recombinant arMP-12ΔNSm21/384 vaccine candidate for sheep, goats and calves.

Author

Boumart Z, Daouam S, Bamouh Z, Jazouli M, Tadlaoui KO, Dungu B, Bettinger G, Watts DM, and Elharrak M

Subjects

Animals, Antibodies, Neutralizing, Cattle, Chlorocebus aethiops, Goats, Immunoglobulin G blood, Immunoglobulin G immunology, Morocco, Neutralization Tests, Sheep, Vaccines, Attenuated administration & dosage, Vaccines, Attenuated adverse effects, Vaccines, Attenuated genetics, Vaccines, Synthetic administration & dosage, Vaccines, Synthetic adverse effects, Vaccines, Synthetic genetics, Vero Cells, Viral Vaccines administration & dosage, Viral Vaccines adverse effects, Viral Vaccines genetics, Virus Replication, Cattle Diseases prevention & control, Immunogenicity, Vaccine, Rift Valley Fever prevention & control, Rift Valley fever virus immunology, Sheep Diseases prevention & control, Vaccines, Attenuated immunology, Vaccines, Synthetic immunology, Viral Vaccines immunology

Abstract

Rift Valley fever (RVF) causes serious health and economic losses to the livestock industry as well as a significant cause of human disease. The prevention of RVF in Africa is a global priority, however, available vaccines have only been partially effective. Therefore, the objective of this study was to evaluate the safety and immunogenicity of a live, attenuated recombinant RVFV arMP-12ΔNSm21/384 nucleotide deletion vaccine candidate in domestic ruminants. Evaluation involved testing to determine the infectivity titer of the vaccine virus in Vero cells for industrial scale up vaccine production. Safety experiments were conducted to determine the potential of the vaccine virus to revert to virulence by serial passages in sheep, the possibility of virus spread from vaccinated sheep and calves to unvaccinated animals, and the potential health effects of administering overdoses of the vaccine to sheep, goats and calves. The immunogenicity of 3 doses of 10 4 , 10 5 and 10 6 Tissue Culture Infectious Doses 50% (TCID 50 ) of the vaccine was assessed in 3 groups of 10 sheep and 3 groups of 10 goats, and doses of 10 5 , 10 6 and 10 7 TCID 50 was evaluated in 3 groups of 10 calves subcutaenous vaccintation. The results showed that the infectivity titer of the vaccine virus was 10 8.4 TCID 50 /ml, that the vaccine did not spread from vaccinated to un-vaccinated animals, there was no evidence of reversion to virulence in sheep and the vaccine overdoses did not cause any adverse effects. The immunogenicity among sheep, goats and calves indicated that doses of 10 4 -10 6 TCID 50 elicited detectable antibody by day 7 post-vaccination (PV) with antibody titers ranging from 0.6 log to 2.1 log on day 14 PV with sustained titers through day 28 PV. Overall, these findings indicated that the RVFV arMP-12ΔNSm21/384 vaccine is a promising candidate for the prevention of RVF among domestic ruminants., (Copyright © 2019 Elsevier Ltd. All rights reserved.)

Published

2019

38. Strategies to increase adoption of animal vaccines by smallholder farmers with focus on neglected diseases and marginalized populations.

Author

Donadeu M, Nwankpa N, Abela-Ridder B, and Dungu B

Subjects

Animals, Humans, Neglected Diseases prevention & control, Animal Diseases prevention & control, Farms economics, Livestock, Neglected Diseases veterinary, Social Marginalization, Vaccines immunology

Abstract

Background: Most smallholder farmers (SHFs) and marginalized populations (MPs) in Africa, Asia, and Latin America depend on livestock for their livelihoods. However, significant numbers of these animals do not achieve their potential, die due to disease, or transmit zoonotic diseases. Existing vaccines could prevent and control some of these diseases, but frequently the vaccines do not reach SHFs, especially MPs, making it necessary for specific vaccine adoption strategies., Principal Findings: Several strategies that have the potential to increase the adoption of animal vaccines by SHFs and MPs have been identified depending on the type of vaccines involved. The strategies differed depending on whether the vaccines were aimed at diseases that cause economic losses, government-controlled diseases, or neglected diseases. The adoption of vaccines for neglected diseases presents a major challenge, because they are mostly for zoonotic diseases that produce few or no clinical signs in the animals, making it more difficult for the farmers to appreciate the value of the vaccines. Strategies can be aimed at increasing the availability of quality vaccines, so that they are produced in sufficient quantity, or aimed at increasing access and demand by SHFs and/or MPs. Some of the strategies to increase vaccine adoption might not provide a definite solution but might facilitate vaccine uptake by decreasing barriers. These strategies are varied and include technical considerations, policy components, involvement by the private sector (local and international), and innovation., Conclusions: Several strategies with the potential to reduce livestock morbidity and mortality, or prevent zoonoses in SHFs communities and MPs through vaccination, require the involvement of donors and international organisations to stimulate and facilitate sustainable adoption. This is especially the case for neglected zoonotic diseases. Support for national and regional vaccine manufacturers is also required, especially for vaccines against diseases of interest only in the developing world and public goods., Competing Interests: The authors have declared that no competing interests exist. The authors alone are responsible for the views expressed in this publication and they do not necessarily represent the decisions, policy or views of their respective employers.

Published

2019

39. Tackling human and animal health threats through innovative vaccinology in Africa.

Author

Warimwe GM, Purushotham J, Perry BD, Hill AVS, Gilbert SC, Dungu B, and Charleston B

Abstract

Africa bears the brunt of many of the world's most devastating human and animal infectious diseases, a good number of which have no licensed or effective vaccines available. The continent's potential to generate novel interventions against these global health threats is however largely untapped. Strengthening Africa's vaccine research and development (R&D) sector could accelerate discovery, development and deployment of effective countermeasures against locally prevalent infectious diseases, many of which are neglected and have the capacity to spread to new geographical settings. Here, we review Africa's human and veterinary vaccine R&D sectors and identify key areas that should be prioritized for investment, and synergies that could be exploited from Africa's veterinary vaccine industry, which is surprisingly strong and has close parallels with human vaccine R&D., Competing Interests: No competing interests were disclosed., (Copyright: © 2018 Warimwe GM et al.)

Published

2018

40. Rift Valley fever vaccines: current and future needs.

Author

Dungu B, Lubisi BA, and Ikegami T

Subjects

Africa epidemiology, Animals, Disease Outbreaks, Rift Valley Fever immunology, Vaccination, Rift Valley Fever prevention & control, Rift Valley fever virus immunology, Viral Vaccines immunology

Abstract

Rift Valley fever (RVF) is a zoonotic mosquito-borne bunyaviral disease associated with high abortion rates, neonatal deaths, and fetal malformations in ruminants, and mild to severe disease in humans. Outbreaks of RVF cause huge economic losses and public health impacts in endemic countries in Africa and the Arabian Peninsula. A proper vaccination strategy is important for preventing or minimizing outbreaks. Vaccination against RVF is not practiced in many countries, however, due to absence or irregular occurrences of outbreaks, despite serological evidence of RVF viral activity. Nonetheless, effective vaccination strategies, and functional national and international multi-disciplinary networks, remain crucial for ensuring availability of vaccines and supporting execution of vaccination in high risk areas for efficient response to RVF alerts and outbreaks., (Copyright © 2018 Elsevier B.V. All rights reserved.)

Published

2018

41. Erratum to: Efficacy of vaccination with La Sota strain vaccine to control Newcastle disease in village chickens in Nepal.

Author

Shrestha S, Dhawan M, Donadeu M, and Dungu B

Published

2017

42. Efficacy of vaccination with La Sota strain vaccine to control Newcastle disease in village chickens in Nepal.

Author

Shrestha S, Dhawan M, Donadeu M, and Dungu B

Subjects

Animals, Antibodies, Viral blood, Antibody Formation, Disease Outbreaks prevention & control, Disease Outbreaks veterinary, Enzyme-Linked Immunosorbent Assay, Hemagglutination Inhibition Tests veterinary, Immunization, Secondary, Nepal, Newcastle disease virus, Vaccines, Attenuated therapeutic use, Chickens immunology, Chickens virology, Newcastle Disease prevention & control, Vaccination veterinary, Viral Vaccines therapeutic use

Abstract

The efficacy of vaccination with Newcastle disease (ND) La Sota and R 2 B (Mukteswar) modified live strain vaccines was determined by experimental challenge and with ND La Sota vaccine under field conditions in Nepal. Booster vaccination with ND La Sota vaccine after a primary vaccination with ND La Sota vaccine, induced a geometric mean titre (GMT) of 5.0 log 2 haemagglutination inhibition (HI) units, compared to a GMT of 6.0 log 2 HI units following booster vaccination with R 2 B vaccine 1 month after primary vaccination with ND La Sota vaccine. Both vaccines provided 100% protection against challenge with a local field ND strain. Furthermore, booster vaccination with ND La Sota vaccine induced protective levels of antibody after field use in villages in Jhapa, and no outbreaks of ND occurred during the study period. The ND La Sota modified live vaccine is immunogenic and efficacious and is a suitable vaccine for use in vaccination programmes in village chickens in the rural areas of Nepal.

Published

2017

43. Development, characterization and optimization of a new suspension chicken-induced pluripotent cell line for the production of Newcastle disease vaccine.

Author

Shittu I, Zhu Z, Lu Y, Hutcheson JM, Stice SL, West FD, Donadeu M, Dungu B, Fadly AM, Zavala G, Ferguson-Noel N, and Afonso CL

Subjects

Animals, Cell Line, Chick Embryo, Chickens, Induced Pluripotent Stem Cells metabolism, Induced Pluripotent Stem Cells virology, Newcastle Disease prevention & control, Newcastle disease virus, Viral Vaccines biosynthesis

Abstract

Traditionally, substrates for production of viral poultry vaccines have been embryonated eggs or adherent primary cell cultures. The difficulties and cost involved in scaling up these substrates in cases of increased demand have been a limitation for vaccine production. Here, we assess the ability of a newly developed chicken-induced pluripotent cell line, BA3, to support replication and growth of Newcastle disease virus (NDV) LaSota vaccine strain. The characteristics and growth profile of the cells were also investigated. BA3 cells could grow in suspension in different media to a high density of up to 7.0 × 10(6) cells/mL and showed rapid proliferation with doubling time of 21 h. Upon infection, a high virus titer of 1.02 × 10(8) EID50/mL was obtained at 24 h post infection using a multiplicity of infection (MOI) of 5. In addition, the cell line was shown to be free of endogenous and exogenous Avian Leukosis viruses, Reticuloendotheliosis virus, Fowl Adenovirus, Marek's disease virus, and several Mycoplasma species. In conclusion, BA3 cell line is potentially an excellent candidate for vaccine production due to its highly desirable industrially friendly characteristics of growing to high cell density and capability of growth in serum free medium., (Published by Elsevier Ltd.)

Published

2016

44. Safety and immunogenicity of Onderstepoort Biological Products' Rift Valley fever Clone 13 vaccine in sheep and goats under field conditions in Senegal.

Author

Lo MM, Mbao V, Sierra P, Thiongane Y, Diop M, Donadeu M, and Dungu B

Subjects

Animals, Female, Goat Diseases immunology, Goats, Male, Pregnancy, Rift Valley Fever immunology, Senegal, Sheep, Sheep Diseases immunology, Vaccines, Attenuated administration & dosage, Viral Vaccines adverse effects, Goat Diseases prevention & control, Rift Valley Fever prevention & control, Rift Valley fever virus immunology, Sheep Diseases prevention & control, Vaccines, Attenuated immunology, Viral Vaccines immunology

Abstract

This blinded field safety study was conducted in Senegal to assess safety and immunogenicity of administration of the registered dose of Rift Valley fever virus (RVFV) Clone 13 vaccine (Onderstepoort Biological Products) to sheep and goats of West African breeds under natural conditions. A total of 267 small ruminants (220 sheep, 47 goats) were included; half received RVFV Clone 13 vaccine at the recommended dose and half received the diluent (as placebo) only. The study was performed on three commercial farms in the northern and eastern region of Senegal in accordance with veterinary good clinical practices. The animals were observed daily for 3 days after vaccination, and then weekly for 1 year. In both sheep and goats vaccinated against RVFV seroconversion rates above 70% were recorded. No seroconversion related to RVFV was observed in placebo-treated animals. No statistically significant differences were determined between placebo and vaccinated groups for mean rectal temperatures for the first 3 days after administration (p > 0.05). No abnormal clinical signs related to treatment were noted, and only one slight injection site reaction was observed in one vaccinated animal for 2 days after vaccination. Out of 176 births assessed over 1 year (93 from the vaccinated group, 83 from the placebo group), 9 were abnormal in the placebo group and 3 in the vaccinated group (p > 0.05). The frequency of adverse events was similar in the placebo and vaccinated groups. RVFV Clone 13 vaccine administered according to the manufacturer's instructions was safe and well tolerated in West African breeds of sheep and goats, including animals of approximately 6 months of age and pregnant females, under field conditions in Senegal. Antibody levels persisted up to 1 year after vaccination.

Published

2015

45. Randomized controlled field trial to assess the immunogenicity and safety of rift valley fever clone 13 vaccine in livestock.

Author

Njenga MK, Njagi L, Thumbi SM, Kahariri S, Githinji J, Omondi E, Baden A, Murithi M, Paweska J, Ithondeka PM, Ngeiywa KJ, Dungu B, Donadeu M, and Munyua PM

Subjects

Animals, Antibodies, Neutralizing blood, Antibodies, Viral blood, Cattle, Female, Goats, Kenya, Livestock, Male, Sheep, South Africa, Viral Vaccines adverse effects, Rift Valley fever virus immunology, Viral Vaccines immunology

Abstract

Background: Although livestock vaccination is effective in preventing Rift Valley fever (RVF) epidemics, there are concerns about safety and effectiveness of the only commercially available RVF Smithburn vaccine. We conducted a randomized controlled field trial to evaluate the immunogenicity and safety of the new RVF Clone 13 vaccine, recently registered in South Africa., Methods: In a blinded randomized controlled field trial, 404 animals (85 cattle, 168 sheep, and 151 goats) in three farms in Kenya were divided into three groups. Group A included males and non-pregnant females that were randomized and assigned to two groups; one vaccinated with RVF Clone 13 and the other given placebo. Groups B included animals in 1st half of pregnancy, and group C animals in 2nd half of pregnancy, which were also randomized and either vaccinated and given placebo. Animals were monitored for one year and virus antibodies titers assessed on days 14, 28, 56, 183 and 365., Results: In vaccinated goats (N = 72), 72% developed anti-RVF virus IgM antibodies and 97% neutralizing IgG antibodies. In vaccinated sheep (N = 77), 84% developed IgM and 91% neutralizing IgG antibodies. Vaccinated cattle (N = 42) did not develop IgM antibodies but 67% developed neutralizing IgG antibodies. At day 14 post-vaccination, the odds of being seropositive for IgG in the vaccine group was 3.6 (95% CI, 1.5 - 9.2) in cattle, 90.0 (95% CI, 25.1 - 579.2) in goats, and 40.0 (95% CI, 16.5 - 110.5) in sheep. Abortion was observed in one vaccinated goat but histopathologic analysis did not indicate RVF virus infection. There was no evidence of teratogenicity in vaccinated or placebo animals., Conclusions: The results suggest RVF Clone 13 vaccine is safe to use and has high (>90%) immunogenicity in sheep and goats but moderate (> 65%) immunogenicity in cattle.

Published

2015

46. Animal trypanosomosis: making quality control of trypanocidal drugs possible.

Author

Sutcliffe OB, Skellern GG, Araya F, Cannavan A, Sasanya JJ, Dungu B, van Gool F, Münstermann S, and Mattioli RC

Subjects

Africa South of the Sahara epidemiology, Animals, Molecular Structure, Trypanocidal Agents chemistry, Trypanosomiasis, African drug therapy, Trypanosomiasis, African epidemiology, Internationality, Trypanocidal Agents therapeutic use, Trypanosomiasis, African veterinary, Veterinary Drugs standards

Abstract

African animal trypanosomosis is arguably the most important animal disease impairing livestock agricultural development in sub-Saharan Africa. In addition to vector control, the use oftrypanocidal drugs is important in controlling the impact of the disease on animal health and production in most sub-Saharan countries. However, there are no internationally agreed standards (pharmacopoeia-type monographs or documented product specifications) for the quality control of these compounds. This means that it is impossible to establish independent quality control and quality assurance standards for these agents. An international alliance between the Food and Agriculture Organization of the United Nations, the International Federation for Animal Health, the Global Alliance for Livestock Veterinary Medicines, the University of Strathclyde and the International Atomic Energy Agency (with critical support from the World Organisation for Animal Health) was established to develop quality control and quality assurance standards for trypanocidal drugs, with the aim of transferring these methodologies to two control laboratories in sub-Saharan Africa that will serve as reference institutions for their respective regions. The work of the international alliance will allow development of control measures against sub-standard or counterfeit trypanocidal drugs for treatment of trypanosome infection. Monographs on diminazene aceturate (synonym: diminazene diaceturate), isometamidium chloride hydrochloride, homidium chloride and bromide salts and their relevant veterinary formulations for these agents are given in the annex to this paper. However, the authors do not recommend use of homidium bromide and chloride, because of their proven mutagenic properties in some animal test models and their suspected carcinogenic properties.

Published

2014

47. Development of a low-dose fast-dissolving tablet formulation of Newcastle disease vaccine for low-cost backyard poultry immunisation.

Author

Lal M, Zhu C, McClurkan C, Koelle DM, Miller P, Afonso C, Donadeu M, Dungu B, and Chen D

Subjects

Animals, Chemistry, Pharmaceutical, Developing Countries, Drug Carriers administration & dosage, Drug Stability, Feasibility Studies, Freeze Drying, Microbial Viability, Poultry, Vaccination economics, Vaccination methods, Viral Vaccines chemistry, Viral Vaccines economics, Newcastle Disease prevention & control, Poultry Diseases prevention & control, Tablets administration & dosage, Vaccination veterinary, Viral Vaccines administration & dosage

Abstract

The immunisation of backyard poultry is critical for maintaining healthy flocks to provide nutrition and income for low-resource farmers worldwide. A vaccine presentation for flocks of less than 50 birds could make it more affordable and accessible, increasing uptake and impact. Fast-dissolving tablets (FDT) of Newcastle disease virus (NDV) vaccine were produced by freeze drying the LaSota NDV strain combined with excipients into tablets containing a small number of doses and packaged in polymer blister sheets. The NDV-FDT vaccine maintained virus stability for more than six months at 4°C, based on plaque assay and egg infectivity dose data. Stability was further confirmed in a challenge study, where the tablet vaccine elicited a strong immune response and provided 100 per cent protection to vaccinated chickens infected with a virulent strain of NDV. The vaccine tablet can be diluted in water (no needle or syringe required) and administered either in drinking water or with a dropper via an intraocular and/or intransal route. Results indicate that FDTs containing a small number of doses are a feasible presentation for backyard poultry farmers. The compact packaging of the FDTs will also provide cost savings in storing and distributing the vaccine in the cold chain., (British Veterinary Association.)

Published

2014

48. Efficacy of a single high oxfendazole dose against gastrointestinal nematodes in naturally infected pigs.

Author

Alvarez L, Saumell C, Fusé L, Moreno L, Ceballos L, Domingue G, Donadeu M, Dungu B, and Lanusse C

Subjects

Animals, Feces parasitology, Gastrointestinal Tract parasitology, Helminthiasis, Animal parasitology, Parasite Egg Count veterinary, Species Specificity, Swine, Swine Diseases parasitology, Antinematodal Agents therapeutic use, Benzimidazoles therapeutic use, Helminthiasis, Animal drug therapy, Nematoda drug effects, Swine Diseases drug therapy

Abstract

The goal of the current experiment was to assess the clinical efficacy of oxfendazole (OFZ) administered as a single oral dose (30 mg/kg) to pigs naturally parasitized with Ascaris suum, Oesophagostomum spp., Metastrongylus spp. and Trichuris suis. Thirty-six local ecotype piglets were divided into three independent experiments, named I, II and III (n=12 each), respectively. Each experiment involved two different groups (n=6): Untreated Control and OFZ treated. Animals were naturally parasitized with A. suum (Experiments I, II and III), Oesophagostomum spp. (Experiments I and II), T. suis (Experiments II and III) and Metastrongylus spp. (Experiment I). Pigs in the treated group received OFZ (Synanthic(®), Merial Ltd., 9.06% suspension) orally at 30 mg/kg dose. At five (5) days post-treatment, animals were sacrificed and the clinical efficacy of the OFZ treatment was established following the currently available WAAVP guidelines for a controlled efficacy test. None of the animals involved in this experiment showed any adverse events during the study. OFZ treatment given as a single 30 mg/kg oral dose showed a 100% efficacy against all the nematode parasites present in the three experiments. In conclusion, under the current experimental conditions, OFZ orally administered to naturally parasitized piglets at a single dose of 30 mg/kg was safe and highly efficacious (100%) against adult stages of A. suum, Oesophagostomum spp., T. suis and Metastrongylus spp., (Copyright © 2013 Elsevier B.V. All rights reserved.)

Published

2013

49. Vaccination for the control of Rift Valley fever in enzootic and epizootic situations.

Author

Dungu B, Donadeu M, and Bouloy M

Subjects

Animals, Disease Outbreaks prevention & control, Global Health, Humans, Immunization Schedule, Rift Valley Fever diagnosis, Rift Valley Fever prevention & control, Vaccination, Disease Outbreaks veterinary, Rift Valley Fever veterinary, Viral Vaccines immunology

Abstract

Vaccination continues to be the most effective way to control Rift Valley fever (RVF), a zoonotic insect-borne viral disease of livestock. The irregular, cyclical and persistent nature of RVF in its occurrence in enzootic situations suggests that the vaccination strategy to be considered for these regions should be different from what is envisaged for free from risk regions. Currently available RVF vaccines have been extensively used for the control of the disease. However, these vaccines have shortcomings that have encouraged many research groups to develop new vaccine candidates that would address a large number of the current challenges, and be suitable for use both in disease-free regions and in different contingency and emergency preparedness strategies. The characteristics of different RVF vaccines and vaccination strategies are discussed in this report.

Published

2013

50. A high oxfendazole dose to control porcine cysticercosis: pharmacokinetics and tissue residue profiles.

Author

Moreno L, Lopez-Urbina MT, Farias C, Domingue G, Donadeu M, Dungu B, García HH, Gomez-Puerta LA, Lanusse C, and González AE

Subjects

Adipose Tissue chemistry, Animals, Anthelmintics administration & dosage, Anthelmintics pharmacokinetics, Area Under Curve, Benzimidazoles administration & dosage, Benzimidazoles pharmacokinetics, Cysticercosis drug therapy, Cysticercosis pathology, Dose-Response Relationship, Drug, Female, Half-Life, Kidney chemistry, Male, Muscle, Skeletal chemistry, Swine, Swine Diseases parasitology, Anthelmintics therapeutic use, Benzimidazoles therapeutic use, Cysticercosis veterinary, Drug Residues analysis, Swine Diseases drug therapy

Abstract

Oxfendazole (OFZ) is efficacious for porcine cysticercosis at 30 mg/kg. OFZ is not registered to be used at this dose. The assessment of the OFZ and metabolites [(fenbendazole sulphone (FBZSO2), fenbendazole (FBZ)] plasma pharmacokinetic and tissue residue profiles after its oral administration to pigs and the withdrawal period for human consumption were reported. Forty-eight pigs allocated into two groups received OFZ (30 mg/kg) orally as a commercial (CF) or as experimental formulation (SMF). Samples (blood, muscle, liver, kidney and fat) were collected over 30 days post-treatment and analyzed by HPLC. OFZ was the main compound recovered in plasma, followed by FBZSO2 and low FBZ concentrations. OFZ AUC0-LOQ (209.9±33.9 μg·h/ml) and Cmax (5.40±0.65 μg/ml) parameters for the CF tended to be higher than those for the SMF (AUC0-LOQ: 159.4±18.3 μg h/ml, Cmax: 3.80±0.35 μg/ml). The highest total residue (OFZ+FBZSO2+FBZ) concentrations were quantified in liver, followed by kidney, muscle and fat tissue. FBZSO2 residue levels were the highest found in muscle (0.68±0.39 μg/g) and fat (0.69±0.39 μg/g). In liver and kidney the highest residues corresponded to FBZ (5.29±4.36 μg/g) and OFZ (2.86±0.75 μg/g), respectively. A withdrawal time of 17 days post-treatment was established before tissues are delivered for human consumption., (Copyright © 2012 Elsevier Ltd. All rights reserved.)

Published

2012