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      Adenovirus 2, Bordetella bronchiseptica, and Parainfluenza Molecular Diagnostic Assay Results in Puppies After vaccination with Modified Live Vaccines

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          Abstract

          Background

          Canine adenovirus 2, parainfluenza, and Bordetella bronchiseptica cause respiratory disease in dogs, and each has a modified live intranasal vaccine available. Molecular diagnostic assays to amplify specific nucleic acids are available for each of these agents. If positive molecular diagnostic assay results are common after vaccination, the positive predictive value of the diagnostic assays for disease would be decreased.

          Objective

          To determine the impact of administration of commercially available modified live topical adenovirus 2, B. bronchiseptica , and parainfluenza vaccine has on the results of a commercially available PCR panel.

          Animals

          Eight puppies from a research breeding facility negative for these pathogens.

          Methods

          Blinded prospective pilot study. Puppies were vaccinated with a single dose of modified live topical adenovirus 2, B. bronchiseptica , and parainfluenza and parenteral dose of adenovirus 2, canine distemper virus, and parvovirus. Nasal and pharyngeal swabs were collected on multiple days and submitted for PCR assay.

          Results

          Nucleic acids of all 3 organisms contained in the topical vaccine were detected from both samples multiple times through 28 days after vaccination with higher numbers of positive samples detected between days 3 and 10 after vaccination.

          Conclusions and Clinical Importance

          Vaccine status should be considered when interpreting respiratory agent PCR results if modified live vaccines have been used. Development of quantitative PCR and wild‐type sequencing are necessary to improve positive predictive value of these assays by distinguishing vaccinate from natural infection.

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          Most cited references8

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          New and emerging pathogens in canine infectious respiratory disease.

          Canine infectious respiratory disease is a common, worldwide disease syndrome of multifactorial etiology. This review presents a summary of 6 viruses (canine respiratory coronavirus, canine pneumovirus, canine influenza virus, pantropic canine coronavirus, canine bocavirus, and canine hepacivirus) and 2 bacteria (Streptococcus zooepidemicus and Mycoplasma cynos) that have been associated with respiratory disease in dogs. For some pathogens a causal role is clear, whereas for others, ongoing research aims to uncover their pathogenesis and contribution to this complex syndrome. Etiology, clinical disease, pathogenesis, and epidemiology are described for each pathogen, with an emphasis on recent discoveries or novel findings.
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            Long-term viremia and fecal shedding in pups after modified-live canine parvovirus vaccination

            Highlights • Dogs were administered type 2 or 2b modified-live canine parvovirus (CPV) vaccines. • Vaccine CPV-2b shedding occurred for a shorter period but with greater viral loads. • Viremia was detected for a longer period and at higher titers for CPV-2b than CPV-2. • CPV seroconvertion occurred earlier with CPV-2b than with CPV-2 vaccines. • Vaccine viruses were detected by PCR but not by antigen testing or hemagglutination.
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              Common and emerging infectious diseases in the animal shelter.

              The beneficial role that animal shelters play is unquestionable. An estimated 3 to 4 million animals are cared for or placed in homes each year, and most shelters promote public health and support responsible pet ownership. It is, nonetheless, inevitable that shelters are prime examples of anthropogenic biological instability: even well-run shelters often house transient, displaced, and mixed populations of animals. Many of these animals have received minimal to no prior health care, and some have a history of scavenging or predation to survive. Overcrowding and poor shelter conditions further magnify these inherent risks to create individual, intraspecies, and interspecies stress and provide an environment conducive to exposure to numerous potentially collaborative pathogens. All of these factors can contribute to the evolution and emergence of new pathogens or to alterations in virulence of endemic pathogens. While it is not possible to effectively anticipate the timing or the pathogen type in emergence events, their sites of origin are less enigmatic, and pathologists and diagnosticians who work with sheltered animal populations have recognized several such events in the past decade. This article first considers the contribution of the shelter environment to canine and feline disease. This is followed by summaries of recent research on the pathogenesis of common shelter pathogens, as well as research that has led to the discovery of novel or emerging diseases and the methods that are used for their diagnosis and discovery. For the infectious agents that commonly affect sheltered dogs and cats, including canine distemper virus, canine influenza virus, Streptococcus spp, parvoviruses, feline herpesvirus, feline caliciviruses, and feline infectious peritonitis virus, we present familiar as well as newly recognized lesions associated with infection. Preliminary studies on recently discovered viruses like canine circovirus, canine bocavirus, and feline norovirus indicate that these pathogens can cause or contribute to canine and feline disease.
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                Author and article information

                Journal
                J Vet Intern Med
                J. Vet. Intern. Med
                10.1111/(ISSN)1939-1676
                JVIM
                Journal of Veterinary Internal Medicine
                John Wiley and Sons Inc. (Hoboken )
                0891-6640
                1939-1676
                Jan-Feb 2016
                22 December 2015
                : 30
                : 1 ( doiID: 10.1111/jvim.2016.30.issue-1 )
                : 164-166
                Affiliations
                [ 1 ] Center for Companion Animal Studies and the Department of Clinical SciencesColorado State University Ft. Collins CO
                [ 2 ]Antech Diagnostics Lake Success NY
                Author notes
                [*] [* ]Corresponding author: R. Ruch‐Gallie, DVM, MS, 300 West Drake Road, Fort Collins, CO 80523; e‐mail: rgallie@ 123456colostate.edu .
                Article
                JVIM13821
                10.1111/jvim.13821
                4913651
                26692461
                8480ac8b-f180-420c-a4b3-910d1e503184
                Copyright © 2015 The Authors. Journal of Veterinary Internal Medicine published by Wiley Periodicals, Inc. on behalf of the American College of Veterinary Internal Medicine .

                This is an open access article under the terms of the Creative Commons Attribution‐NonCommercial License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited and is not used for commercial purposes.

                History
                : 29 June 2015
                : 08 October 2015
                : 24 November 2015
                Page count
                Pages: 3
                Categories
                Standard Article
                SMALL ANIMAL
                Standard Articles
                Infectious Disease
                Custom metadata
                2.0
                jvim13821
                January/February 2016
                Converter:WILEY_ML3GV2_TO_NLMPMC version:4.9.1 mode:remove_FC converted:17.06.2016

                Veterinary medicine
                canine,polymerase chain reaction,respiratory,shelter
                Veterinary medicine
                canine, polymerase chain reaction, respiratory, shelter

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