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犬猫的年龄与长期保护性免疫

Age and long-term protective immunity in dogs and cats.

作者信息

Schultz R D, Thiel B, Mukhtar E, Sharp P, Larson L J

机构信息

Department of Pathobiological Sciences, School of Veterinary Medicine, University of Wisconsin-Madison, Madison, Wisconsin, USA.

出版信息

J Comp Pathol. 2010 Jan;142 Suppl 1:S102-8. doi: 10.1016/j.jcpa.2009.10.009. Epub 2009 Dec 3.

Abstract

Vaccination can provide an immune response that is similar in duration to that following a natural infection. In general, adaptive immunity to viruses develops earliest and is highly effective. Such anti-viral immune responses often result in the development of sterile immunity and the duration of immunity (DOI) is often lifelong. In contrast, adaptive immunity to bacteria, fungi or parasites develops more slowly and the DOI is generally short compared with most systemic viral infections. Sterile immunity to these infectious agents is less commonly engendered. Old dogs and cats rarely die from vaccine-preventable infectious disease, especially when they have been vaccinated and immunized as young adults (i.e. between 16 weeks and 1 year of age). However, young animals do die, often because vaccines were either not given or not given at an appropriate age (e.g. too early in life in the presence of maternally derived antibody [MDA]). More animals need to be vaccinated to increase herd (population) immunity. The present study examines the DOI for core viral vaccines in dogs that had not been revaccinated for as long as 9 years. These animals had serum antibody to canine distemper virus (CDV), canine parvovirus type 2 (CPV-2) and canine adenovirus type-1 (CAV-1) at levels considered protective and when challenged with these viruses, the dogs resisted infection and/or disease. Thus, even a single dose of modified live virus (MLV) canine core vaccines (against CDV, cav-2 and cpv-2) or MLV feline core vaccines (against feline parvovirus [FPV], feline calicivirus [FCV] and feline herpesvirus [FHV]), when administered at 16 weeks or older, could provide long-term immunity in a very high percentage of animals, while also increasing herd immunity.

摘要

疫苗接种可产生一种免疫反应,其持续时间与自然感染后的免疫反应相似。一般来说,对病毒的适应性免疫最早产生且非常有效。这种抗病毒免疫反应通常会导致无菌免疫的形成,免疫持续时间(DOI)往往是终身的。相比之下,对细菌、真菌或寄生虫的适应性免疫发展较慢,与大多数全身性病毒感染相比,其DOI通常较短。对这些病原体产生无菌免疫的情况较少见。老年犬猫很少死于疫苗可预防的传染病,尤其是当它们在年轻时(即16周龄至1岁之间)已接种疫苗并获得免疫时。然而,幼龄动物确实会死亡,通常是因为未接种疫苗或未在合适的年龄接种(例如,在存在母源抗体[MDA]的情况下过早接种)。需要给更多动物接种疫苗以提高群体(种群)免疫力。本研究检测了长达9年未再次接种疫苗的犬只中核心病毒疫苗的DOI。这些动物体内犬瘟热病毒(CDV)、犬细小病毒(CPV-2)和犬腺病毒1型(CAV-1)的血清抗体水平被认为具有保护性,当用这些病毒进行攻击时,这些犬只抵抗了感染和/或疾病。因此,即使是单剂量的改良活病毒(MLV)犬用核心疫苗(针对CDV、CAV-2和CPV-2)或MLV猫用核心疫苗(针对猫细小病毒[FPV]、猫杯状病毒[FCV]和猫疱疹病毒[FHV]),在16周龄或更大年龄接种时,也能在很高比例的动物中提供长期免疫力,同时还能提高群体免疫力。

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