K. B. Chua scite author profile

Nipah virus, a newly identified paramyxovirus caused a severe outbreak of encephalitis in Malaysia with high fatalities. We report an open-label trial of ribavirin in 140 patients, with 54 patients who were managed prior to the availability of ribavirin or refused treatment as control. There were 45 deaths (32%) in the ribavirin arm; 29 deaths (54%) occurred in the control arm. This represents a 36% reduction in mortality (p = 0.011). There was no associated serious side effect. This study suggests that ribavirin is able to reduce the mortality of acute Nipah encephalitis.

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Molecular epidemiology of enterovirus 71 in peninsular Malaysia, 1997?2000

Herrero

Lee

Hurrelbrink

et al. 2003

Archives of Virology

100

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Human enterovirus 71 (EV71) (genus Enterovirus, family Picornaviridae) has been responsible for sporadic cases and outbreaks of hand-foot-and-mouth disease (HFMD), aseptic meningitis, encephalitis and poliomyelitis-like disease in Europe, the U.S.A., Australia and Asia. Recently, there has been an increase in EV71 activity in the Asia-Pacific region, with many outbreaks of HFMD associated with brainstem encephalitis manifesting as neurogenic pulmonary oedema with a high case fatality rate. In 1997, and again in 2000, EV71 outbreaks occurred in peninsular Malaysia. Variations in VP1 gene sequences have been shown to divide all known EV71 field isolates into three distinct genogroups (A, B and C). Consequently we examined the VP1 gene sequences of 43 EV71 strains isolated in peninsular Malaysia between 1997 and 2000 in order to determine the genogroup prevalence over the period. In this study we show that four subgenogroups (B3, B4, C1 and C2) of EV71 circulated in peninsular Malaysia between 1997 and 2000. Subgenogroups B3, B4 and C1 have been identified as the primary cause of the outbreaks of EV71 in peninsular Malaysia. Subgenogroup C1 also displayed endemic circulation from 1997 to 2000 and subgenogroup C2 was present at a low level during the 1997 outbreak.

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The Presence of Nipah Virus in Respiratory Secretions and Urine of Patients during an Outbreak of Nipah Virus Encephalitis in Malaysia

Chua

Lam

Goh

et al. 2001

Journal of Infection

140

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Neurogenic pulmonary oedema and enterovirus 71 encephalomyelitis

et al. 1998

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Molecular phylogeny of modern coxsackievirus A16

et al. 2007

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A phylogenetic analysis of VP1 and VP4 nucleotide sequences of 52 recent CVA16 strains demonstrated two distinct CVA16 genogroups, A and B, with the prototype strain being the only member of genogroup A. CVA16 G-10, the prototype strain, showed a nucleotide difference of 27.7-30.2% and 19.9-25.2% in VP1 and VP4, respectively, in relation to other CVA16 strains, which formed two separate lineages in genogroup B with nucleotide variation of less than 13.4% and less than 16.3% in VP1 and VP4, respectively. Lineage 1 strains circulating before 2000 were later displaced by lineage 2 strains.

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Complete nucleotide sequences of Nipah virus isolates from Malaysia

Chan

Chua

Koh

et al. 2001

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Viral aetiology of lower respiratory tract infection in young Malaysian children

Chan

Goh²,

Chua

et al. 1999

J Paediatr Child Health

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Comparison of the complete nucleotide sequences of echovirus 7 strain UMMC and the prototype (Wallace) strain demonstrates significant genetic drift over time

Chua

McMinn²,

Lam

et al. 2001

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The complete nucleotide sequences are reported of two strains of echovirus 7, the prototype Wallace strain (Eo7-Wallace) and a recent Malaysian strain isolated from the cerebrospinal fluid of a child with fatal encephalomyelitis (Eo7-UMMC strain). The molecular findings corroborate the serological placement of the UMMC strain as echovirus 7. Both Eo7-Wallace and Eo7-UMMC belong to the species human enterovirus B and are most closely related to echovirus 11. Eo7-UMMC has undergone significant genetic drift from the prototype strain in the 47 years that separate the isolation of the two viruses. Phylogenetic analysis revealed that Eo7-UMMC did not arise from recombination with another enterovirus serotype. The molecular basis for the severely neurovirulent phenotype of Eo7-UMMC remains unknown. However, it is shown that mutations in the nucleotide sequence of the 5h untranslated region (UTR) of Eo7-UMMC result in changes to the putative structure of the 5h UTR. It is possible that these changes contribute to the neurovirulence of Eo7-UMMC.

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K. B. Chua

Treatment of acute Nipah encephalitis with ribavirin

Molecular epidemiology of enterovirus 71 in peninsular Malaysia, 1997?2000

The Presence of Nipah Virus in Respiratory Secretions and Urine of Patients during an Outbreak of Nipah Virus Encephalitis in Malaysia

Neurogenic pulmonary oedema and enterovirus 71 encephalomyelitis

Molecular phylogeny of modern coxsackievirus A16

Complete nucleotide sequences of Nipah virus isolates from Malaysia

Viral aetiology of lower respiratory tract infection in young Malaysian children

Comparison of the complete nucleotide sequences of echovirus 7 strain UMMC and the prototype (Wallace) strain demonstrates significant genetic drift over time

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