Human parainfluenza viruses (HPIVs) are the viruses that cause human parainfluenza. HPIVs are a paraphyletic group of four distinct single-stranded RNA viruses belonging to the Paramyxoviridae family. These viruses are closely associated with both human and veterinary disease.[2] Virions are approximately 150–250 nm in size and contain negative sense RNA with a genome encompassing about 15,000 nucleotides.[3]
The viruses can be detected via cell culture, immunofluorescent microscopy, and PCR.[4] HPIVs remain the second main cause of hospitalisation in children under 5 years of age for a respiratory illness (only respiratory syncytial virus (RSV) causes more respiratory hospitalisations for this age group).[5]
Classification
editThe first HPIV was discovered in the late 1950s. The taxonomic division is broadly based on antigenic and genetic characteristics, forming four major serotypes or clades, which today are considered distinct viruses.[6] These include:
Virus | GenBank acronym | NCBI taxonomy | Notes |
---|---|---|---|
Human parainfluenza virus type 1 | HPIV-1 | 12730 | Most common cause of croup |
Human parainfluenza virus type 2 | HPIV-2 | 11212 | Causes croup and other upper and lower respiratory tract illnesses |
Human parainfluenza virus type 3 | HPIV-3 | 11216 | Associated with bronchiolitis and pneumonia |
Human parainfluenza virus type 4 | HPIV-4 | 11203 | Includes subtypes 4a and 4b |
HPIVs belong to two genera: Respirovirus (HPIV-1 & HPIV-3) and Rubulavirus (HPIV-2 & HPIV-4).[3]
Viral structure and organisation
editHPIVs are characterised by producing enveloped virions and containing single stranded negative sense RNA.[3] Non-infectious virions have also been reported to contain RNA with positive polarity.[3] HPIV genomes are about 15,000 nucleotides in length and encode six key structural proteins.[3]
The structural gene sequence of HPIVs is as follows: 3′-NP-P-M-F-HN-L-5′ (the protein prefixes and further details are outlined in the table below).[7]
Structural protein | Location | Function |
---|---|---|
Hemagglutinin-neuraminidase (HN) | Envelope | Attachment and cell entry |
Fusion Protein (F) | Envelope | Fusion and cell entry |
Matrix Protein (M) | Within the envelope | Assembly |
Nucleoprotein (NP) | Nucleocapsid | Forms a complex with the RNA genome |
Phosphoprotein (P) | Nucleocapsid | Forms as part of RNA polymerase complex |
Large Protein (L) | Nucleocapsid | Forms as part of RNA polymerase complex |
With the advent of reverse genetics, it has been found that the most efficient human parainfluenza viruses (in terms of replication and transcription) have a genome nucleotide total that is divisible by the number 6. This has led to the "rule of six" being coined. Exceptions to the rule have been found, and its exact advantages are not fully understood.[8]
Electrophoresis has shown that the molecular weight of the proteins for the four HPIVs are similar (with the exception of the phosphoprotein, which shows significant variation).[3][9]
Viral entry and replication
editViral replication is initiated only after successful entry into a cell by attachment and fusion between the virus and the host cell lipid membrane. Viral RNA (vRNA) is initially associated with nucleoprotein (NP), phosphoprotein (P) and the large protein (L). The hemagglutinin–neuraminidase (HN) is involved with viral attachment and thus hemadsorption and hemagglutination. Furthermore, the fusion (F) protein is important in aiding the fusion of the host and viral cellular membranes, eventually forming syncytia.[10]
Initially the F protein is in an inactive form (F0) but can be cleaved by proteolysis to form its active form, F1 and F2, linked by di-sulphide bonds. Once complete, this is followed by the HPIV nucleocapsid entering the cytoplasm of the cell. Subsequently, genomic transcription occurs using the viruses own 'viral RNA-dependent RNA polymerase' (L protein). The cell's own ribosomes are then tasked with translation, forming the viral proteins from the viral mRNA.[10]
Towards the end of the process, (after the formation of the viral proteins) the replication of the viral genome occurs. Initially, this occurs with the formation of a positive-sense RNA (intermediate step, necessary for producing progeny), and finally, negative-sense RNA is formed which is then associated with the nucleoprotein. This may then be either packaged and released from the cell by budding or used for subsequent rounds of transcription and replication.[11]
The observable and morphological changes that can be seen in infected cells include the enlargement of the cytoplasm, decreased mitotic activity and 'focal rounding', with the potential formation of multi-nucleate cells (syncytia).[12]
The pathogenicity of HPIVs is mutually dependent on the viruses having the correct accessory proteins that are able to elicit anti-interferon properties. This is a major factor in the clinical significance of disease.[11]
Host range
editThe main host remains the human. However, infections have been induced in other animals (both under natural and experimental situations), although these were always asymptomatic.[13]
Clinical significance
editIt is estimated that there are 5 million children with lower respiratory infections (LRI) each year in the United States alone.[14] HPIV-1, HPIV-2 and HPIV-3 have been linked with up to a third of these infections.[15] Upper respiratory infections (URI) are also important in the context of HPIV, however, they are caused to a lesser extent by the virus.[16] The highest rates of serious HPIV illnesses occur among young children, and surveys have shown that about 75% of children aged 5 or older have antibodies to HPIV-1.[citation needed]
For infants and young children, it has been estimated that about 25% will develop "clinically significant disease".[17]
Repeated infection throughout the life of the host is not uncommon and symptoms of later breakouts include upper respiratory tract illness, such as cold and a sore throat.[3] The incubation period for all four serotypes is 1 to 7 days.[18] In immunosuppressed people, parainfluenza virus infections can cause severe pneumonia, which can be fatal.[19]
HPIV-1 and HPIV-2 have been demonstrated to be the principal causative agent behind croup (laryngotracheobronchitis), which is a viral disease of the upper airway and is mainly problematic in children aged 6–48 months of age.[20][21] Biennial epidemics starting in autumn are associated with both HPIV-1 and -2; however, HPIV-2 can also have yearly outbreaks.[14] Additionally, HPIV-1 tends to cause biennial outbreaks of croup in the fall. In the United States, large peaks have presently been occurring during odd-numbered years.[citation needed]
HPIV-3 has been closely associated with bronchiolitis and pneumonia, and principally targets those aged <1 year.[22]
HPIV-4 remains infrequently detected. It is now believed to be more common than previously thought but less likely to cause severe disease. By the age of 10, the majority of children are seropositive for HPIV-4 infection—this may be indicative of a large proportion of asymptomatic or mild infections.[3]
Those with compromised immunity have a higher risk of infection and mortality and may fall ill with more extreme forms of LRI.[13] Associations between HPIVs and neurologic disease are known. For example, hospitalisation with certain HPIVs has a strong association with febrile seizures.[23] HPIV-4b has the strongest association (up to 62%)[vague] followed by HPIV-3 and -1.[3]
HPIVs have also been linked with rare cases of viral meningitis[24] and Guillain–Barré syndrome.[12]
HPIVs are spread from person to person (i.e., horizontal transmission) by contact with infected secretions in respiratory droplets or contaminated surfaces or objects. Infection can occur when infectious material contacts the mucous membranes of the eyes, mouth, or nose, and possibly through the inhalation of droplets generated by a sneeze or cough. HPIVs can remain infectious in airborne droplets for over an hour.[citation needed]
Airway inflammation
editThe inflammation of the airway is a common attribute of HPIV infection. It is believed to occur due to the large scale upregulation of inflammatory cytokines. Common cytokines observed to be upregulated include IFN–α, various interleukins (i.e., IL–2, IL-6), and TNF–α. Various chemokines and inflammatory proteins are also believed to be associated with the common symptoms of HPIV infection.[12]
Recent evidence suggests that the virus-specific antibody immunoglobulin E may be responsible for mediating the large-scale releases of histamine in the trachea that are believed to cause croup.[12][25]
Immunology
editThe body's primary defense against HPIV infection is adaptive immunity involving both humoral and cellular immunity. With humoral immunity, antibodies that bind to the surface viral proteins HN and F protect against later infection.[26] Patients with defective cell-mediated immunity also experience more severe infection, suggesting that T cells are important in clearing infection.[12]
Diagnosis
editDiagnosis can be made in several ways, encompassing a range of multi-faceted techniques:[4]
- Isolation and detection of the virus in cell culture.
- Detection of viral antigens directly within bodily respiratory tract secretions using immunofluorescence, enzyme immunoassays or fluoroimmunoassays.
- Polymerase chain reaction (PCR).
- Analysis of specific IgG antibodies showing a subsequent rise in titre following infection (using paired serum specimens).
Because of the similarity in terms of the antigenic profile between the viruses, hemagglutination assay (HA) or hemadsorption inhibition (HAdI) processes are often used. Both complement fixation, neutralisation, and enzyme linked immunosorbent assays – ELISA, can also be used to aid in the process of distinguishing between viral serotypes.[3]
Morbidity and mortality
editMortality caused by HPIVs in developed regions of the world remains rare. Where mortality has occurred, it is principally in the three core risk groups (very young, elderly and immuno-compromised). Long-term changes can however be associated with airway remodeling and are believed to be a significant cause of morbidity.[27] The exact associations between HPIVs and diseases such as chronic obstructive pulmonary disease (COPD) are still being investigated.[28]
In developing regions of the world, preschool children remain the highest mortality risk group. Mortality may be a consequence of primary viral infection or secondary problems, such as bacterial infection. Predispositions, such as malnutrition and other deficiencies, may further elevate the chances of mortality associated with infection.[12]
Overall, LRIs cause approximately 25–30% of total deaths in preschool children in the developing world. HPIVs are believed to be associated with 10% of all LRI cases, thus remaining a significant cause of mortality.[12]
Risk factors
editNumerous factors have been suggested and linked to a higher risk of acquiring the infection, inclusive of malnutrition, vitamin A deficiency, absence of breastfeeding during the early stages of life, environmental pollution and overcrowding.[29]
Prevention
editDespite decades of research, no vaccines currently exist.[30]
Recombinant technology has however been used to target the formation of vaccines for HPIV-1, -2 and -3 and has taken the form of several live-attenuated intranasal vaccines. Two vaccines in particular were found to be immunogenic and well tolerated against HPIV-3 in phase I trials. HPIV-1 and -2 vaccine candidates remain less advanced.[17]
Vaccine techniques which have been used against HPIVs are not limited to intranasal forms, but also viruses attenuated by cold passage, host range attenuation, chimeric construct vaccines and also introducing mutations with the help of reverse genetics to achieve attenuation.[31]
Maternal antibodies may offer some degree of protection against HPIVs during the early stages of life via the colostrum in breast milk.[32]
Medication
editRibavirin is one medication which has shown good potential for the treatment of HPIV-3 given recent in-vitro tests (in-vivo tests show mixed results).[12] Ribavirin is a broad-spectrum antiviral, and as of 2012, was being administered to those who are severely immuno-compromised, despite the lack of conclusive evidence for its benefit.[12] Protein inhibitors and novel forms of medication have also been proposed to relieve the symptoms of infection.[13]
Furthermore, antibiotics may be used if a secondary bacterial infection develops. Corticosteroid treatment and nebulizers are also a first line choice against croup if breathing difficulties ensue.[12]
Interactions with the environment
editParainfluenza viruses last only a few hours in the environment and are inactivated by soap and water. Furthermore, the virus can also be easily destroyed using common hygiene techniques and detergents, disinfectants and antiseptics.[4]
Environmental factors which are important for HPIV survival are pH, humidity, temperature and the medium within which the virus is found. The optimal pH is around the physiologic pH values (7.4 to 8.0), whilst at high temperatures (above 37 °C) and low humidity, infectivity reduces.[33]
The majority of transmission has been linked to close contact, especially in nosocomial infections. Chronic care facilities and doctors' surgeries are also known to be transmission 'hotspots' with transmission occurring via aerosols, large droplets and also fomites (contaminated surfaces).[34]
The exact infectious dose remains unknown.[13]
Economic burden
editIn economically disadvantaged regions of the world, HPIV infection can be measured in terms of mortality. In the developed world where mortality remains rare, the economic costs of the infection can be estimated. Estimates from the US are suggestive of a cost (based on extrapolation) in the region of $200 million per annum.[3]
Differences between influenza and parainfluenza
editInfluenza viruses belong to the Orthomyxoviridae family; Parainfluenza viruses (HPIVs) belong to the Paramyxoviridae family. Influenza typically causes more severe illness than parainfluenza. While both can cause upper respiratory symptoms, influenza is more likely to result in high fever, body aches, and fatigue. Parainfluenza often produces milder, cold-like symptoms such as runny nose, cough, and low-grade fever.[35] Influenza has a distinct seasonal pattern, with outbreaks occurring mainly in winter months. Parainfluenza viruses circulate year-round, with each type having its own seasonal patterns. The viruses have a tendency towards different complications: influenza is more likely to cause severe pneumonia in high-risk groups; parainfluenza is more likely to cause croup in children. Influenza has effective vaccines available and can be treated with antiviral medications like neuraminidase inhibitors. There are currently no vaccines or specific antiviral treatments for parainfluenza viruses. Parainfluenza tends to infect young children, with most children being infected by age 5. Influenza can affect all ages.[36][37]
References
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- ^ a b c "Human Parainfluenza Viruses". Centers for Disease Control and Prevention (2011). Archived from the original on 20 March 2012. Retrieved 21 March 2012.
- ^ Schmidt, Alexander; Anne Schaap-Nutt; Emmalene J Bartlett; Henrick Schomacker; Jim Boonyaratanakornkit; Ruth A Karron; Peter L Collins (1 February 2011). "Progress in the development of human parainfluenza virus vaccines". Expert Review of Respiratory Medicine. 5 (4): 515–526. doi:10.1586/ers.11.32. PMC 3503243. PMID 21859271.
- ^ Baron, S.; Enders, G. (1996). "Paramyxoviruses". Parainfluenza Viruses. University of Texas Medical Branch at Galveston. ISBN 9780963117212. PMID 21413341. Retrieved 2009-03-15.
- ^ Hunt, Dr. Margaret. "PARAINFLUENZA, RESPIRATORY SYNCYTIAL AND ADENO VIRUSES". Reference.MD. Retrieved 21 March 2012.
- ^ Vulliémoz, D; Roux, L (May 2001). "'Rule of six': how does the Sendai virus RNA polymerase keep count?". Journal of Virology. 75 (10): 4506–4518. doi:10.1128/JVI.75.10.4506-4518.2001. PMC 114204. PMID 11312321.
- ^ Henrickson, K. J (2003). "Parainfluenza Viruses". Clinical Microbiology Reviews. 16 (2): 242–264. doi:10.1128/CMR.16.2.242-264.2003. PMC 153148. PMID 12692097.
- ^ a b Moscona, A (July 2005). "Entry of parainfluenza virus into cells as a target for interrupting childhood respiratory disease". The Journal of Clinical Investigation. 115 (7): 1688–1698. doi:10.1172/JCI25669. PMC 1159152. PMID 16007245.
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- ^ Denny, FW; Clyde WA, Jr (May 1986). "Acute lower respiratory tract infections in nonhospitalized children". The Journal of Pediatrics. 108 (5 Pt 1): 635–46. doi:10.1016/S0022-3476(86)81034-4. PMID 3009769.
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- ^ a b Durbin, AP; Karron, RA (December 15, 2003). "Progress in the development of respiratory syncytial virus and parainfluenza virus vaccines". Clinical Infectious Diseases. 37 (12): 1668–1677. doi:10.1086/379775. PMID 14689350. S2CID 41967381.
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- ^ HAMBLING, MH (December 1964). "Survival of the Respiratory Syncytial Virus During Storage Under Various Conditions". British Journal of Experimental Pathology. 45 (6): 647–55. PMC 2093680. PMID 14245166.
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- ^ "About Human Parainfluenza Viruses (HPIVs)". CDC. November 11, 2024.
- ^ Henrickson, Kelly J. (April 2003). "Parainfluenza Viruses". Clinical Microbiology Reviews. 16 (2): 242–264. doi:10.1128/CMR.16.2.242-264.2003. ISSN 0893-8512. PMC 153148. PMID 12692097.
- ^ Sharland, Mike; Butler, Karina; Cant, Andrew; Dagan, Ron, eds. (April 2016), "Influenza and parainfluenza", OSH Manual of Childhood Infections, Oxford University Press, pp. 628–632, doi:10.1093/med/9780198729228.003.0080, ISBN 978-0-19-872922-8, retrieved 2024-11-13
Further reading
edit- Henrickson KJ (2003). "Parainfluenza viruses". Clin. Microbiol. Rev. 16 (2): 242–64. doi:10.1128/cmr.16.2.242-264.2003. PMC 153148. PMID 12692097.
- Human Parainfluenza Viruses (HPIVs)
External links
edit- Human Parainfluenza Viruses – information provided by the CDC