Abstract
Human parechovirus (HPeV), especially HPeV A3 (HPeV3), causes sepsis-like diseases and sudden infant death syndrome in neonates and young infants. Development of rapid and easier diagnostic laboratory tests for HPeVs is desired. Original inner primers, outer primers, and loop-primers were designed on the 5' untranslated region of HPeV3. HPeV3 ribonucleic acids (RNAs), other viral RNAs, and clinical stool samples were used to confirm whether the designed primers would allow the detection of HPeV3 with the reverse transcription loop-mediated isothermal amplification (RT-LAMP) technique. Three combinations of primers were created and it was confirmed that all primer sets allowed the detection of HPeV3 RNAs. The primer sets had cross-reactivity with HPeV type 1 (HPeV1), but all sets showed negative results when applied to coxsackievirus, echovirus, enterovirus, norovirus, and adenovirus genomes. Four of six stool samples, obtained from newborn and infant patients with sepsis-like symptoms, showed positive results with our RT-LAMP technique. This manuscript is the first description of an RT-LAMP for the diagnosis of HPeVs, allowing a faster, easier, and cheaper diagnosis. This technique is clinically useful for newborns and infants who have sepsis-like symptoms.
Highlights
Human parechovirus (HPeV) is increasingly being recognized as a potentially severe viral infection in neonates and young infants [1,2,3]
Three combinations of primers were created and it was confirmed that all primer sets allowed the detection of Human parechovirus A3 (HPeV3) ribonucleic acids (RNAs)
The primer sets had cross-reactivity with HPeV type 1 (HPeV1), but all sets showed negative results when applied to coxsackievirus, echovirus, enterovirus, norovirus, and adenovirus genomes
Summary
Human parechovirus (HPeV) is increasingly being recognized as a potentially severe viral infection in neonates and young infants [1,2,3]. Human parechovirus A3 (HPeV3) is the most clinically important genotype among HPeVs because of its association with severe disease in newborns and young infants [1, 3]. HPeV3-infected infants can present with a sepsis-like symptom, often with central nervous system involvement, which is difficult to differentiate clinically from bacterial sepsis [1, 3]. They may present with fever, tachycardia, and erythema [1]. Severe HPeV3 infection in infants is associated with a risk of long-term complications [1]
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