Introduction Nonpolio enteroviruses (EV) cause serious diseases and associated with high mortality rate in neonates. Several factors for severe EV infection were reported. Whether some enterovirus strains caused fatal disease and some only caused nonspecific febrile illness is not clear. In this study, we used echovirus 11 as a representative and aimed to investigate replication capacity of echovirus 11 strains isolated from patients with severe complication and with nonspecific febrile. In addition, clinical and laboratory data of patients with all types enterovial infection were analyzed to figure out differences between severe and mild neonatal EV infections. Methods This retrospective study was conducted in Mackay Memorial and Children Hospital and National Taiwan University Children Hospital. Patients aged ≤ 30 days with culture or PCR proved EV infections were collected from January 2008 to December 2018. Demographic and laboratory date of patients was recorded and analyzed. We obtained echovirus 11 strains isolated from patients with severe complication and from nonspecific febrile. Viral strains were cultured in Rhabdomyosarcoma (RD) cell for propagation and measured titer by plaque assays. Then, growth curves of echovirus 11 strains were performed at 37℃ and 39.5℃ and harvest for quantified by real-time quantitative PCR (qRT-PCR). Two-sample t-test and Chi-square test was performed for statistics. A p < 0.05 was considered statistically significant. Results We collected 113 patients and 61 (54.0%) patients was in nonspecific febrile illness group. Forty-two (37.2%) had aseptic meningitis and 10 patients had myocarditis or hepatic necrosis with coagulopathy including in severe group. There were two fatal cases. WBC counts at admission and maximum WBC counts during hospitalization both higher in severe group (p=0.0039 and 0.0004, respectively). The disease onset of patients in severe group was younger than in severe group (p=0.022). The viral load of 4 echovirus 11 strains cultured at 39.5℃ was lower than that at 37℃ harvested at 24 hours and 36 hours post infection. Comparing severe and mild stains cultured at 39.5℃ and 37℃, respectively, viral load were not significant different at measured time points. Conclusion The onset of disease is younger in patients with severe complication than in that with nonspecific febrile illness. The fatal cases decreased comparing to previous study in Taiwan. The replication capacity of echovirus 11 strains was inhibited at 39℃. Determinants of EV virulent in neonates require further research.