Paramyxoviridae - Overview
Introduction
The Paramyxoviridae have a helical nucleocapsid surrounded by an envelope comprised of host cell membrance spiked with viral glycoproteins responsible for haemagglutinin, neuraminidase and haemolytic activities. The genome of the Paramyxoviridae is single-stranded, negative-sense RNA which is used as a template for the production of messenger (positive-sense) RNA and further genomic material. Paramyxoviridae are sensitive to heat, dessication and most disinfectants, and so are not resistant in the environment. The Paramyxovididae family is divided to two sub-families, the Paramyxovirinae and the Pneumovirinae. It is within the Paramyxovirinae sub-family that morbilliviruses fall, along with respiroviruses, henipaviruses, rubulaviruses and avulaviruses. As well as canine distemper virus (CDV), the morbilliviruses include rinderpest, peste de petits ruminants, measles, phocine distemper and dolphin distemper.
Morphology
- Single-stranded negative-sense unsegmented RNA virus
- Reassortment and antigenic shift cannot occur
- Spike proteins include
- HN (Haemagglutinin and Neuraminidase)
- F (Fusion glycoprotein), which allows the virus to fuse directly to the plasma membrane and release its RNA
- F also causes syncitium to form, which aids diagnosis
- Host antibody response to the F protein is the basis for vaccination
Virulence
- Paramyxoviruses replicate in the epithelium of the upper respiratory tract as well as occasionally in the gut
- Sites of spike protein cleavage
- Virulence varies by virus, see below
Types and Subtypes
Paramoyxoviridae was reclassified in 2000 to include 2 subfamilies and 5 genera, of interest including:
- Subfamily: Paramyxovirinae:
- Subfamily: Pneumovirinae
Antigenic Variation
- Antigenic conservation allows some cross protection by vaccination:
- Conservation of major virus-specific F/HN antigens means vaccines protect against all isolates of the same virus
- Minor morbillivirus-specific epitopes on F allows some cross protection between canine distemper, measles, and rinderpest
- Antigenic "fingerprinting" is possible for some viruses based on minor variable epitopes of HN, F and NP on specific isolates as detected by monoclonal antibodies
- These are detected by immunostaining infected cells