Systematic Reviews
Copyright ©The Author(s) 2016.
World J Hepatol. Mar 28, 2016; 8(9): 452-460
Published online Mar 28, 2016. doi: 10.4254/wjh.v8.i9.452
Table 1 Food and drug administration pregnancy categories for hepatitis B virus antiviral therapy[15]
Pregnancy categorydefinitionHBV therapy categorization
AAdequate and well controlled studies have failed to demonstrate a risk to the fetus in the first trimester of pregnancy (and there is no evidence of risk in later trimesters)None
BAnimal reproduction studies have failed to demonstrate a risk to the fetus, and there are no adequate and well-controlled studies in pregnant women or animal studies that have shown an adverse effect, but adequate and well-controlled studies in pregnant women have failed to demonstrate a risk to the fetus in any trimesterTelbivudine; Tenofovir
CAnimal reproduction studies have shown an adverse effect on the fetus, and there are no adequate and well controlled studies in humans, but potential benefits might warrant use of the drug in pregnant women despite potential risksLamivudine; Entecavir; Adefovir
DThere is positive evidence of human fetus risk based on adverse reaction data from investigational or marketing experience or studies in humans, but potential benefits might warrant use of the drug in pregnant women despite potential risksNone
XStudies in animals or humans have demonstrated fetus abnormalities, and/or there is positive evidence of human fetus risk based on adverse reaction data from investigational or marketing experience, and the risks involved in use of the drug in pregnant women clearly outweigh potential benefitsInterferon
Table 2 Reproductive and developmental toxicity with telbivudine
Study typeRoute of administrationSpeciesNo. of animalsDoses (mg/kg per day)TreatmentReference
Rat studies
Fertility, reproduction,Oral gavageSprague Dawley rats25 males0, 100, 500, 1000Males: -28 AC to DG 17Study 1314-001
developmental25 femalesFemales: -15 AC to DG 17
FertilityOral gavageSprague Dawley rats25 males0, 1000, 2000Males: -28 AC to DG 13Study 1314-005
25 females
FertilityOral gavageSprague Dawley rats25 males0, 2000Females: -15 AC to DG 7Study 1314-006
25 females
Peri/postnatalOral gavageSprague Dawley rats25 females0, 100, 250, 1000Females: DG 7 to DL 20Study 1314-003
Rabbit study
DevelopmentalOral gavageNew Zealand White rabbits20 females0, 50, 250, 1000Females: DG 6-18Study 1314-002
AC: Ante coitum; DG: Gestation day; DL: Lactation day.
Table 3 Non-overlapping literature references of telbivudine exposure during pregnancy
Ref.Original languageStudy designLdT starting trimester during pregnancyNo. of pregnancy with exposure to LdTMaternal HBV DNA (at inclusion)
Chen et al[46]ChineseProspective1st trimester43≥ 1 × 107 copies/mL
Han et al[47]EnglishProspective2nd and 3rd trimesters362> 1.0 × 106 copies/mL
Jiang et al[53]ChineseProspective3rd trimesters28> 103 copies/mL (at inclusion)
Liu et al[38]ChineseProspective3rd trimester5≥ 1 × 107 copies/mL (before treatment)
Liu et al[28]EnglishProspective1st trimester89> 1 × 105 copies/mL
Liu et al[21]EnglishProspective1st, 2nd or 3rd trimesters82≥ 106 IU/mL
Mohan et al[54]EnglishProspective1st trimester14.0433 × 104 copies/mL
Peng et al[39]ChineseProspective3rd trimester40≥ 1 × 106 copies/mL
Wu et al[27]EnglishProspective2nd or 3rd trimester279> 106 IU/mL
Yu et al[44]EnglishProspective1st, 2nd or 3rd trimester233> 1.0 × 106 copies/mL
Zeng et al[40]ChineseProspective3rd trimester22≥ 105 copies/mL
Zeng et al[22]EnglishProspective1st or 3rd trimester54Not reported
Zhao et al[55]ChineseProspective3rd trimester30Not reported
Zhang et al[41]ChineseProspective3rd trimester31> 1 × 107 copies/mL
Zhang et al[42]ChineseProspective3rd trimester60≥ l × 106 copies/mL
Zhang et al[26]EnglishProspective3rd trimester257> 6 log10 copies/mL
Zhou et al[43]ChineseProspective3rd trimester36≥ 1 × 107 copies/mL
Zhou et al[45]ChineseProspective1st trimester73≥ 1 × 107 copies/mL
Table 4 Summary of prevalence rates of birth defects, abortion and perinatal transmission rates with telbivudine exposure during pregnancy in literature studies
Events (n)Population (N)Rate in telbivudine treated patients (n/N)Non-antiviral treatment control in literature studiesBackground rates in overall population (prevalence based on surveillance reports)
Birth defects: Live birth prevalence616733.6/1000a3.0/100014.5-60/10001
Birth defects: Birth prevalence616733.6/1000a3.0/1000NA
Birth defects: Total prevalence716744.2/1000b3.0/1000NA
Spontaneous abortion716824.2/1000NA16/10002
Elective termination116820.6/1000NA230/10003
MTCT1115720.70% (11/1572)d11.9% (124/1041)10%-15%4
1EUROCAT data[48]; MACDP data[49]; Christianson et al[50] (2006); Dai et al[34] (2011);
2US CDC data[51];
3WHO data[52];
4Historical data from HBV-infected population without antiviral treatment[10-12].
aP = 1.0000 vs non-antiviral treatment control in the same literature studies (Fisher’s exact test);
bP = 0.7502 vs non-antiviral treatment control in the same literature studies (Fisher’s exact test);
dP < 0.0001 vs non-antiviral treatment control in the same literature studies (Fisher’s exact test). NA: Not available; MTCT: Mother-to-child transmission.