1). The characteristics of the HCV-RNA+ve infants and their parents are described in Table 1. The rate of HCV-VT was higher for infants born to mothers with high HCV viremia (>600,000 IU/mL) than for infants born to mothers with low HCV viremia (<600,000; Table 2; P = 0.02). Neither gender, nor weight, nor viral genotype (genotype 1 versus genotype non-1), nor type of birth (cesarean versus noncesarean), nor breast-feeding were associated with increased risk of HCV-VT. None of the
infected infants were HCV-RNA-positive at birth and the mean age at the first HCV-RNA-positive result was 3.81 ± 0.91 months. The infected children presented a lower birth weight (nonsignificant) than that of the noninfected children. 37% of the noninfected children Napabucasin in vivo presented ALT levels > 40 U/L whereas 68% of the infected infants had high levels of ALT (>40 U/L, P = 0.016). The study of risk factors for chronic infection was performed in HIV-negative mothers using a stored blood sample (Study Cohort, Fig. 1). Fourteen of the 22 HCV-VT-infected infants (64%) cleared the HCV virus spontaneously (transient viremia group) and eight infants (36%) had persistent infection (chronic group). The rate
of HCV chronic infection was higher among the infants with viral genotype 1 than among those with genotype non-1 (Table 3; P = 0.02). In fact, no chronic infection selleck kinase inhibitor was noted in the infants with genotype non-1 (n = 7, of whom six had genotype 3 and one had genotype 4), whereas only 1/9 infants with genotype non-1 in the general cohort had persistent infection at the end of the study (this infant was a boy whose mother was genotype 3 but HIV-positive). Neither gender, nor weight, nor the mother’s HCV viral load, nor the type of birth (cesarean versus noncesarean), nor breast-feeding were associated with increased selleck inhibitor risk of HCV chronic infection among these infants.
Among the HCV chronic group of infants, the first HCV-RNA-positive result was recorded at a mean age of 2.33 ± 0.3 months, whereas the corresponding value for the transient viremia group was 4.15 ± 1.1 months (nonsignificant). Furthermore, the chronic HCV infants had a lower birth weight than did the transient viremia children (nonsignificant). In all, 50% of the infants with transient viremia presented ALT levels >40 U/L, whereas all the chronic infants presented ALT levels above 40 U/L (P = 0.02). This study was performed among the HIV-negative mothers using a stored blood sample (n = 105, Study Cohort; Fig. 1. In six mothers it was not possible to determine the IL28B polymorphism). Of the 31 mothers with IL28B CC polymorphism, 19 were HCV-RNA-positive (61%), whereas among the 68 mothers with non-CC polymorphism (CT or TT polymorphism), 56 were HCV-RNA-positive (82%). Accordingly, the mothers with non-CC IL28B polymorphism had a greater probability of being HCV-RNA-positive than did those with CC polymorphism (OR = 2.95; 95% CI: 1.1-7.7; P = 0.026).