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Characterization of group B coxsackieviruses isolated from non-polio acute flaccid paralysis patients in Pakistan: vital assessment before polio eradication

Published online by Cambridge University Press:  25 July 2017

M. ANGEZ
Affiliation:
Department of Virology, National Institute of Health, Chak Shahzad, Park Road, Islamabad-45500, Pakistan Department of Microbiology, Faculty of Biological Sciences, Quaid-i-Azam University, Islamabad-45320, Pakistan
S. SHAUKAT*
Affiliation:
Department of Virology, National Institute of Health, Chak Shahzad, Park Road, Islamabad-45500, Pakistan
R. ZAHRA
Affiliation:
Department of Microbiology, Faculty of Biological Sciences, Quaid-i-Azam University, Islamabad-45320, Pakistan
M. M. ALAM
Affiliation:
Department of Virology, National Institute of Health, Chak Shahzad, Park Road, Islamabad-45500, Pakistan
S. SHARIF
Affiliation:
Department of Virology, National Institute of Health, Chak Shahzad, Park Road, Islamabad-45500, Pakistan
A. KHURSHID
Affiliation:
Department of Virology, National Institute of Health, Chak Shahzad, Park Road, Islamabad-45500, Pakistan
Y. ARSHAD
Affiliation:
Department of Virology, National Institute of Health, Chak Shahzad, Park Road, Islamabad-45500, Pakistan
M. SULEMAN
Affiliation:
Department of Virology, National Institute of Health, Chak Shahzad, Park Road, Islamabad-45500, Pakistan
G. MUJTABA
Affiliation:
Department of Virology, National Institute of Health, Chak Shahzad, Park Road, Islamabad-45500, Pakistan
S. S. Z. ZAIDI
Affiliation:
Department of Virology, National Institute of Health, Chak Shahzad, Park Road, Islamabad-45500, Pakistan
*
*Author for correspondence: S. Shaukat, Department of Virology, National Institute of Health, Chak Shahzad, Park Road, Islamabad-45500, Pakistan. (Email: vibgyors@yahoo.com)
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Summary

Pakistan is at the verge of polio eradication but isolation of non-polio enteroviruses (NPEVs) from acute flaccid paralysis (AFP) cases may result in serious or even fatal outcome. Many enteroviruses share similar symptoms and epidemiology as is the case with poliovirus and coxsackievirus (CV). The present study was designed to genetically characterize coxsackievirus B (CV-B) serotypes isolated from non-polio acute flaccid paralytic children, as well as to understand their probable role in paralysis. A total of 63 (20·1%) out of 313 stool samples during 2013 were found positive for NPEVs in rhabdomyosarcoma cells. Only 24 (38·0%) NPEVs were typed as CV-B by microneutralization assay and were further characterized by sequencing of the viral protein 1 (VP1) gene. Molecular phylogenetic analyses classified the study strains into six coxsackievirus B serotypes (coxsackievirus B1 to B6) with their respective prototype strains with evidence of epidemiological linkage and distinct clusters. Moreover, four major differences were found within the amino acid sequences of BC-loop in VP1 of CV-B strains. In conclusion, this study presented the molecular evolutionary genetic overview and distinct phylogenetic pattern of CV-B isolates from AFP cases in Pakistan, and explored the possible link between CV-B infections and AFP cases. Furthermore, our data reveal that these viruses might contribute to the incidence of paralysis in population and there is need of time to establish an enterovirus surveillance system for better understanding of epidemiological and virological characteristics of NPEV infections associated with AFP cases in the country.

Information

Type
Original Papers
Copyright
Copyright © Cambridge University Press 2017 
Figure 0

Table 1. Clinical and demographic data of acute flaccid paralytic patients with CV-B infection characterized in this study

Figure 1

Fig. 1. A Phylogenetic tree based on partial VP1 coding sequence of 24 coxsackievirus B strains including CV-B1 to B6 and representative sequences of coxsackievirus serotypes retrieved from GenBank (accession numbers are included in the virus names). Neighbor-joining (NJ) method in MEGA 5·0 was used and evaluated with 1000 bootstrap pseudo-replicates. Bootstrap values greater than 50 are indicated at the respective nodes and the scale bar represents the evolutionary distance. Clusters are marked on the tree. The isolates from this study and prototype strains are represented by ‘●’ and ‘▲’ taxon markers, respectively.

Figure 2

Table 2. Summary of pairwise nucleotide and amino acid sequence comparisons among coxsackievirus B isolates

Figure 3

Fig. 2. Alignment of deduced amino acid sequences of the VP1 polyprotein of CV-B1 to B6 strains with their respective prototype sequence showing only the BC Loop with flanking regions. The sequences within the rectangle show variable sites within the BC-loop region. Strain designations are on the left-hand side of the alignment. Dots (.) represent amino acids identical with respect to CV-B1 to B6 prototype strain and the amino acid symbols indicate where unrelated amino acids exist with reference to prototype strain. In sequence logo the height of the logo at each site is equal to the total information at that site and the height of each symbol in the logo is proportional to its contribution to the information content.