Frontiers in Microbiology (May 2019)

Molecular Epidemiology and Clinical Features of Rotavirus Infection Among Pediatric Patients in East Java, Indonesia During 2015–2018: Dynamic Changes in Rotavirus Genotypes From Equine-Like G3 to Typical Human G1/G3

  • Alpha Fardah Athiyyah,
  • Alpha Fardah Athiyyah,
  • Takako Utsumi,
  • Takako Utsumi,
  • Rury Mega Wahyuni,
  • Zayyin Dinana,
  • Laura Navika Yamani,
  • Soetjipto,
  • Subijanto Marto Sudarmo,
  • Subijanto Marto Sudarmo,
  • Reza Gunadi Ranuh,
  • Reza Gunadi Ranuh,
  • Andy Darma,
  • Andy Darma,
  • Juniastuti,
  • Dadik Raharjo,
  • Chieko Matsui,
  • Lin Deng,
  • Takayuki Abe,
  • Yen Hai Doan,
  • Yoshiki Fujii,
  • Hiroyuki Shimizu,
  • Kazuhiko Katayama,
  • Maria Inge Lusida,
  • Ikuo Shoji

DOI
https://doi.org/10.3389/fmicb.2019.00940
Journal volume & issue
Vol. 10

Abstract

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Group A rotavirus (RVA) is the most important cause of severe gastroenteritis among children worldwide, and effective RVA vaccines have been introduced in many countries. Here we performed a molecular epidemiological analysis of RVA infection among pediatric patients in East Java, Indonesia, during 2015–2018. A total of 432 stool samples were collected from hospitalized pediatric patients with acute gastroenteritis. None of the patients in this cohort had been immunized with an RVA vaccine. The overall prevalence of RVA infection was 31.7% (137/432), and RVA infection was significantly more prevalent in the 6- to 11-month age group than in the other age groups (P < 0.05). Multiplex reverse transcription-PCR (RT-PCR) revealed that the most common G-P combination was equine-like G3P[8] (70.8%), followed by equine-like G3P[6] (12.4%), human G1P[8] (8.8%), G3P[6] (1.5%), and G1P[6] (0.7%). Interestingly, the equine-like strains were exclusively detected until May 2017, but in July 2017 they were completely replaced by a typical human genotype (G1 and G3), suggesting that the dynamic changes in RVA genotypes from equine-like G3 to typical human G1/G3 in Indonesia can occur even in the country with low RVA vaccine coverage rate. The mechanism of the dynamic changes in RVA genotypes needs to be explored. Infants and children with RVA-associated gastroenteritis presented more frequently with some dehydration, vomiting, and watery diarrhea, indicating a greater severity of RVA infection compared to those with non-RVA gastroenteritis. In conclusion, a dynamic change was found in the RVA genotype from equine-like G3 to a typical human genotype. Since severe cases of RVA infection were prevalent, especially in children aged 6 to 11 months or more generally in those less than 2 years old, RVA vaccination should be included in Indonesia’s national immunization program.

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