Skip to main content
PMC home page
BMC Infectious Diseases logoLink to BMC Infectious Diseases
. 2014 May 20;14:277. doi: 10.1186/1471-2334-14-277

The second generation of HIV-1 vertically exposed infants: a case series from the Italian Register for paediatric HIV infection

Carmelina Calitri 1, Clara Gabiano 1, Luisa Galli 2, Elena Chiappini 2, Carlo Giaquinto 3, Wilma Buffolano 4, Orazio Genovese 5, Susanna Esposito 6, Stefania Bernardi 7, Maurizio De Martino 2, Pier-Angelo Tovo 1,, the Italian Register for HIV Infection in Children
PMCID: PMC4035828  PMID: 24885649

Abstract

Background

In the Highly Active Antiretroviral Therapy (HAART) era, the prognosis of children perinatally infected with HIV-1 has significantly improved, so the number of perinatally-infected females entering child-bearing age and experiencing motherhood is increasing.

Methods

A description of the medical history and pregnancy outcomes of women with perinatal acquired HIV-1 infection enrolled in the Italian Register for HIV infection in Children.

Results

Twenty-three women had 29 pregnancies. They had started an antiretroviral therapy at a median of 7.7 years (interquartile range, IQR 2.3 - 11.4), and had experienced a median of 4 therapeutic regimens (IQR 2–6). Twenty women (87%) had taken zidovudine (AZT) before pregnancy, in 14 cases as a starting monotherapy. In 21 pregnancies a protease inhibitor-based regimen was used. At delivery, the median of CD4+ T lymphocytes was 450/μL (IQR 275–522), and no viral load was detectable in 15 cases (reported in 21 pregnancies). Twenty-eight children were delivered through caesarean section (median gestational age: 38 weeks, IQR 36–38, median birth weight: 2550 grams, IQR 2270 – 3000). Intravenous AZT was administered during delivery in 26 cases. All children received oral AZT (median: 42 days, IQR 31 – 42), with no adverse events reported. No child acquired HIV-1 infection.

Conclusions

Despite a long history of maternal infection, multiple antiretroviral regimens and, perhaps, the development of drug-resistant viruses, the risk of mother-to-child transmission does not seem to have increased among the second-generation of HIV-1 exposed infants.

Keywords: HIV-1, Drug-resistant virus, AZT, Vertical transmission

Background

The introduction of Highly Active Antiretroviral Therapy (HAART) has significantly improved the quality of life and prognosis of children with perinatally acquired HIV-1 infection in resource-rich countries [1,2]. As a result, an increasing number of these children are entering adolescence and young adulthood, with a consequent proportion of females becoming sexually active and pregnant. These mothers presented with a long history of HIV-1 infection and sometimes AIDS complications. They had a wide exposition to antiretroviral (ART) drugs and to their, primarily metabolic, chronic side effects. They experienced multiple ART regimens, which were often sub-therapeutic until the advent of HAART, with a consequent risk of acquiring drug-resistant viruses.

Therefore, it has since become crucial to define the pregnancy outcome and effectiveness of ART therapy in preventing mother-to-child HIV-1 transmission (MTCT) in this 2nd generation of HIV-1 exposed infants. Reports from Europe [3,4], Puerto Rico [5], India [6], USA [7-10], and Brazil [11] describe favourable maternal and neonatal outcomes, with a MTCT rate varying from 0 to 7.7%, detected in cases of poor adherence to therapy [10].

Here, we describe the clinical aspects of pregnancy in women with perinatally acquired HIV-1 infection enrolled over the years in the Italian Register for HIV Infection in Children.

Methods

The Italian Register for HIV infection in children (ITLR) is a nationwide, multicentre, prospective study set up by the Italian Association of Paediatrics in 1985. At the moment of patient’s enrolment, written informed consent is obtained from the patient’s guardians; data are treated anonymously as each patient is identified by an alphanumerical code. The study was approved by the review boards and ethics committees of each participating institution, as described in detail elsewhere [1,12]. A retrospective analysis of perinatally HIV-1 infected females, enrolled in the ITLR from its institution and who had a child, was carried out. Information included: the women’s demographic and clinical characteristics, such as their mothers’ risk factors for HIV-1 infection, perinatal ART use, HIV-1 related diseases and comorbidities; the number and types of ART regimens both before and during pregnancy; age at delivery, number of CD4+ T-lymphocytes and viral load at delivery, the mode of delivery; infants’ characteristics (gestational age, sex, birth weight, congenital malformations, any other acute or chronic diseases, adverse events for MTCT prophylaxis, HIV-1 infection status). SPSS (version 20.0) software for Windows was used for data management.

Results

Between 2001 and 2012, 29 children were born to 23 women with perinatal HIV-1 infection. One woman had 3 pregnancies and four women had 2 pregnancies each. See Tables  1, 2 and 3 for data concerning mother-child pairs.

Table 1.

Characteristics of HIV-1 vertically infected women

N. Birth order Risk factors for HIV infection in grandmothers Year of birth Age (years) at start of ART therapy AZT monotherapy No of regimens experienced Years of ART therapy (before the first pregnancy) Clinical and immunological category at last observation Age (years) at AIDS onset Age (years) at delivery
Case 1
 1st
 Drug abuse
 1982
 14.6
 No
 4
 13.2
 A 1
  
 28.4
Case 2
 1st
 Sexual intercourse with drug abuser, Drug abuse
 1982
 10.6
 Yes
 5
 7.7
 B 3
  
 24.6
 
 2nd
  
  
  
  
  
  
  
  
 26.9
Case 3
 1st
 Risk sexual intercourse
 1983
 7.7
 Yes
 6
 17.5
 B 3
  
 26.1
Case 4
 1st
 Drug abuse
 1983
 11.4
 Yes
 7
 7
 B 3
  
 23.9
Case 5
 1st
 Unknown
 1983
 21.7
 No
 1
 0
 B 3
  
 22
 
 2nd
  
  
  
  
  
  
  
  
 23.7
 
 3th
  
  
  
  
  
  
  
  
 24.7
Case 6
 1st
 Drug abuse
 1984
 6.6
 Yes
 6
 9.7
 B 2
  
 17
 
 2nd
  
  
  
  
  
  
  
  
 18.3
Case 7
 1st
 Sexual intercourse with drug abuser
 1985
 3.1
 No
 2
 20.5
 N 2
  
 24.3
Case 8
 1st
 Drug abuse
 1985
 3
 Yes
 15
 17.7
 C 3
 11.5
 22.4
Case 9
 1st
 Sexual intercourse with drug abuser, Drug abuse
 1986
 12.2
 No
 2
 9.5
 C 2
 13.1
 22.2
Case 10
 1st
 Sexual intercourse with drug abuser
 1986
 6.6
 Yes
 6
 14.8
 C 3
 6.6
 22.1
Case 11
 1st
 Unknown
 1986
 10.2
 No
 6
 11.1
 A 3
  
 22
Case 12
 1st
 Sexual intercourse with drug abuser
 1986
 10
 Yes
 3
 6.3
 A 2
  
 21.1
 
 2nd
  
  
  
  
  
  
  
  
 22.2
Case 13
 1st
 Unknown
 1986
 13.3
 No
 1
 11
 A 1
  
 25
Case 14
 1st
 Sexual intercourse with drug abuser
 1987
 2.3
 Yes
 3
 21.6
 B 2
  
 24.5
Case 15
 1st
 Unknown
 1988
 14.4
 No
 2
 10.3
 B 1
  
 22.6
Case 16
 1st
 Unknown
 1988
 1.9
 Yes
 2
 6.2
 A 2
  
 19.2
Case 17
 1st
 Sexual intercourse with drug abuser
 1989
 1.8
 Yes
 5
 18
 A 1
  
 20.3
Case 18
 1st
 Sexual intercourse with drug abuser, Drug abuse
 1990
 1.7
 Yes
 5
 14.4
 B 2
  
 20.1
Case 19
 1st
 Drug abuse
 1990
 5.4
 Yes
 8
 13.9
 B 3
  
 20
Case 20
 1st
 Unknown
 1990
 8.6
 No
 4
 11.6
 A 3
  
 20.8
 
 2nd
  
  
  
  
  
  
  
  
 21.7
Case 21
 1st
 Sexual intercourse with drug abuser
 1991
 1.2
 Yes
 3
 17.3
 B 1
  
 19.3
Case 22
 1st
 Drug abuse
 1991
 0.6
 Yes
 7
 19.2
 C 3
 0.2
 20.4
Case 23 1st Sexual intercourse with drug abuser, Drug abuse 1991 8.2 No 2 9.9 A 2   20
Open in a new tab

Legend. ART = antiretroviral; AZT = zidovudine.

Table 2.

Pregnancy features

N. Birth order ART therapy at conception ART therapy interruption at first trimester ART regimen during pregnancy Gestational week at start Gestational week at end CD4+ at delivery VL at delivery AZT intrapartum Type of delivery
Case 1
 1st
 No
 No
 AZT + 3TC + ATV/rtv
 5
 37
 525
 Undetectable
 Yes
 EC
Case 2
 1st
 Yes
 Yes (from 5th to 12th week)
 DDI + 3TC + NVP
 1
 4
 480
 157
 Yes
 EC
 
  
  
  
 AZT + 3TC + NVP
 13
 38
  
  
  
  
 
 2nd
 Yes
 No
 FTC + TDF + FPV/rtv
 1
 38
 520
 Undetectable
 Yes
 EC
Case 3
 1st
 Yes
 No
 FTC + TDF + ATV/rtv
 1
 38
 125
 Undetectable
 Yes
 EC
Case 4
 1st
 No
 No
 No
  
  
 Unknown
 Unknown
 Yes
 EC
Case 5
 1st
 No
 No
 AZT + 3TC + LPV/rtv
 23
 34
 307
 Unknown
 Yes
 EC
 
 2nd
 Yes
 No
 AZT + 3TC + LPV/rtv
 1
 37
 480
 15332
 Yes
 EC
 
 3th
 Yes
 No
 AZT + 3TC + LPV/rtv
 1
 Unknown
 Unknown
 Unknown
 Yes
 EC
Case 6
 1st
 No
 No
 AZT + 3TC + NVP
 6
 36
 Unknown
 Unknown
 No
 EC
 
 2nd
 No
 No
 AZT + 3TC + NVP
 6
 40
 Unknown
 Unknown
 No
 EC
Case 7
 1st
 Yes
 No
 ABC + 3TC + ATV
 1
 34
 323
 Undetectable
 Yes
 EC
 
  
  
  
 ABC + 3TC + ATV/rtv
 35
 38
  
  
  
  
Case 8
 1st
 Yes
 No
 FTC + TDF + DRV/rtv
 1
 38
 450
 Undetectable
 Yes
 EC
Case 9
 1st
 Yes
 No
 ABC + DDI + LPV/rtv
 1
 16
 312
 7653
 Yes
 EC
 
  
  
  
 AZT + 3TC + LPV/rtv
 17
 36
  
  
  
  
Case 10
 1st
 Yes
 Yes (from 6th to 12th week)
 FTC + TDF + EFV
 1
 5
 240
 Undetectable
 Yes
 EC
 
  
  
  
 AZT + 3TC + LPV/rtv
 13
 38
  
  
  
  
Case 11
 1st
 Unknown
 No
 ABC + TDF + LPV/rtv
 Unknown
 39
 Unknown
 Undetectable
 Yes
 EC
Case 12
 1st
 No
 No
 No
  
  
 Unknown
 Unknown
 Yes
 UC
 
 2nd
 Yes
 No
 AZT + 3TC + LPV/rtv
 1
 38
 95
 Unknown
 Yes
 EC
Case 13
 1st
 Yes
 No
 FTC + NVP
 1
 39
 673
 Undetectable
 Yes
 EC
Case 14
 1st
 Yes
 No
 AZT + 3TC + ABC
 1
 35
 564
 Undetectable
 Yes
 EC
Case 15
 1st
 Yes
 No
 FTC + TDF + DRV/rtv
 1
 37
 501
 Undetectable
 Yes
 EC
Case 16
 1st
 No
 No
 FTC + TDF + ATV/rtv
 16
 36
 522
 Undetectable
 Yes
 EC
Case 17
 1st
 No
 No
 FTC + TDF + ATV
 13
 37
 770
 Undetectable
 Yes
 EC
Case 18
 1st
 Yes
 No
 3TC
 1
 28
 440
 13099
 Yes
 LC
 
  
  
  
 FTC + TDF + DRV/rtv
 29
 36
  
  
  
  
Case 19
 1st
 No
 No
 FTC + TDF + ATV/rtv
 6
 38
 501
 Undetectable
 Yes
 EC
Case 20
 1st
 No
 No
 FTC + TDF + DRV/rtv + RAL
 38
 40
 200
 Undetectable
 Yes
 EC
 
 2nd
 Unknown
 Unknown
 Unknown
  
  
 99
 Unknown
 Unknown
 Unknown
Case 21
 1st
 Yes
 No
 FTC + TDF + ATV/rtv
 1
 38
 776
 615
 Yes
 EC
Case 22
 1st
 Yes
 No
 AZT + DDI + LPV/rtv
 1
 35
 435
 Undetectable
 Yes
 EC
Case 23
 1st
 Yes
 Yes (from 3rd to 9th week)
 FTC + TDF + LPV/rtv
 1
 3
 275
 20000
 Yes
 EC
        FTC + TDF + LPV/rtv 10 38        
Open in a new tab

Legend. VL: viral load (copies/ml); AZT: zidovudine; 3TC: lamivudine; ABC: abacavir; FTC: emtricitabine; TDF: tenofovir; DDI: didanosine; NVP: nevirapine; LPV: lopinavir; ATV: atazanavir; FPV: fosamprenavir; DRV: darunavir; rtv: ritonavir booster; RAL: raltegravir; EC = elective caesarean section; UC = unspecified caesarean section; LC = caesarean section after labour.

Table 3.

HIV-1 exposed children features

N. Birth order Year of birth Gender Gestational age (weeks) Weight at birth (grams)   ART prophylaxis Duration of postnatal ART prophylaxis (days) HIV-1 status Other pathological conditions
Case 1
 1st
 2010
 M
 37
 2590
  
 AZT
 42
 SR
  
Case 2
 1st
 2007
 F
 38
 2550
  
 AZT
 45
 SR
  
 
 2nd
 2009
 M
 38
 3240
  
 AZT
 19
 SR
  
Case 3
 1st
 2009
 F
 38
 3100
  
 AZT
 28
 SR
  
Case 4
 1st
 2007
 F
 38
 2920
  
 AZT
 36
 SR
  
Case 5
 1st
 2005
 F
 34
 1975
  
 AZT
 42
 SR
  
 
 2nd
 2007
 F
 37
 1960
 SGA
 AZT
 42
 SR
 HCV infection
 
 3th
 2008
 F
 Unknown
 Unknown
  
 AZT
 28
 SR
  
Case 6
 1st
 2001
 F
 36
 1880
 SGA
 AZT
 44
 SR
  
 
 2nd
 2002
 F
 40
 3080
  
 AZT
 42
 SR
  
Case 7
 1st
 2009
 M
 38
 2530
  
 AZT
 42
 SR
  
Case 8
 1st
 2008
 F
 38
 2450
  
 AZT
 43
 SR
  
Case 9
 1st
 2008
 F
 36
 2520
  
 AZT
 42
 SR
  
Case 10
 1st
 2008
 M
 38
 3250
  
 AZT
 31
 SR
  
Case 11
 1st
 2008
 F
 39
 2770
  
 AZT
 41
 SR
  
Case 12
 1st
 2007
 M
 35
 2270
  
 AZT + 3TC + NVP
 31
 SR
  
 
 2nd
 2008
 M
 38
 3000
  
 AZT + 3TC + NVP
 42
 SR
  
Case 13
 1st
 2011
 M
 39
 3100
  
 AZT
 41
 SR
  
Case 14
 1st
 2011
 F
 35
 1190
 SGA
 AZT
 18
 SR
  
Case 15
 1st
 2011
 M
 37
 3190
  
 AZT
 42
 SR
  
Case 16
 1st
 2008
 F
 36
 2760
  
 AZT
 42
 SR
  
Case 17
 1st
 2009
 M
 37
 2520
  
 AZT
 29
 SR
 Cryptorchidism
Case 18
 1st
 2010
 M
 36
 2180
  
 AZT
 42
 SR
  
Case 19
 1st
 2010
 F
 38
 2500
  
 AZT
 14
 SR
  
Case 20
 1st
 2011
 F
 40
 2380
 SGA
 AZT
 45
 SR
  
 
 2nd
 2012
 F
 Unknown
 Unknown
  
 Unknown
 Unknown
 SR
  
Case 21
 1st
 2010
 F
 38
 2750
  
 AZT
 42
 SR
  
Case 22
 1st
 2012
 M
 35
 2160
  
 AZT
 42
 SR
  
Case 23 1st 2011 M 38 2690   AZT 33 SR  
Open in a new tab

Legend. M = male; F = female; AZT = zidovudine; 3TC = lamivudine; NVP = nevirapine; SR = seroreverter; SGA= small for gestational age.

The median maternal age at first delivery was 22 years (interquartile range (IQR) 20.1-24.3); the oldest mother was born in 1982, the youngest in 1991. No infected mother was perinatally exposed to antiretroviral drugs, as ART prophylaxis was not used at that time. The grandmothers’ risk factors for HIV-1 infection were known for 17 women: 11 had had high risk sexual intercourse and 6 had been IV drug users. All but one woman had ART therapy during childhood or adolescence. The median age at the start of ART therapy was 7.7 years (IQR 2.3-11.4). The median number of regimens for each woman was 4 (IQR 2–6). Twenty (87%) women were given zidovudine (AZT), in 14 cases as a starting monotherapy for a median period of 4.4 years (IQR 2.0-5.2); 12/14 patients were later shifted to a dual therapy containing AZT (median period 2.4 years, IQR 1.0-3.4). All but 2 women received HAART before pregnancy, with a combination of 3 or more drugs, containing at least one protease-inhibitor (PI) in 16 cases. The median time of the mothers’ exposure to ART drugs before their first pregnancy was 11.6 years (IQR 9.5-17.5). Four women developed an AIDS defining condition (at a median age of 9.0 years, IQR 1.8-12.7); 10 women were classified, according to the CDC paediatric classification, in clinical category B, 8 in category A, 1 in category N. As far as the immunological status is concerned, 5 were in category 1, 8 in category 2, and 10 in category 3.

Ten mothers did not have any ART therapy at the time of conception; of the ten, 2 continued without therapy throughout their pregnancy, 4 started ART therapy in the first trimester and 4 after the 12th week of gestation, including one woman who started a rescue therapy including the integrase inhibitor raltegravir at the 38th week of gestation. In the other pregnancies, the women were already undergoing ART treatment at conception, and 3 of them discontinued therapy in the first trimester (see Table  2). In one case, efavirenz (EFV) was continued during the first 5 weeks of gestation, with a switch to a lopinavir/ritonavir containing combination after the 12th week. A PI-based regimen was used in a total of 21 pregnancies. No complications related to pregnancy were noticed. There was a median of 450/μL (IQR 275–522)CD4+ T lymphocytes at the last check before delivery (reported in 23 of the 29 pregnancies); all women with a previous AIDS-defining condition had > 200 CD4+/μL. The viral load at delivery (reported in 21 pregnancies) was undetectable in 15 cases. Intravenous AZT was administered during 26 (89.6%) deliveries. Twenty-eight children were born through caesarean section, which was elective in 26 cases. No neonatal complications for children at birth were reported; 17 (58.6%) were females; their median gestational age was 38 weeks (IQR 36–38) and the median birth weight was 2550 grams (IQR 2270–3000). Eight were preterm (<37 weeks of gestation), and 4 were small for the gestational age (SGA) (Table  3) [13]. No infant was breastfed. Twenty-six infants received oral AZT as MTCT prophylaxis; 2 brothers received a combined regimen (AZT + 3TC + NVP single dose): the first child because of lack of maternal ART therapy during pregnancy, the second one because of severe maternal immunosuppression (CD4+ T-lymphocytes at labour: 95 cell/ μL). Neonatal ART prophylaxis was administered for a median period of 42 days (IQR 31–42) with no major adverse events.

No child acquired HIV-1 infection. One patient was HCV infected and one presented cryptorchidism. The median age at the last check was 3 years (IQR 1.3-4.3), with nine children followed over 4 years of age.

Discussion

There are few studies exploring the pregnancy outcome in HIV-1 perinatally-infected women. Despite the limited number of pregnancies enrolled and limited amount of available data, ours is one of the largest cohorts with detailed information on the entire maternal history.

The results are reassuring, since none of the 29 exposed infants acquired the infection. Indeed, of the 134 children born to HIV-1 perinatally-infected mothers described in this and other studies [3-11], only 2 acquired the infection, for a total MTCT rate of 1.5%, comparable to that observed in the first-generation of exposed infants with the adoption of the same preventive measures, such as ART therapy during pregnancy, elective caesarean section, ART prophylaxis in the child, and bottle-feeding [12,14,15].

Among 601 women with perinatally acquired HIV-1 infection enrolled in the ITLR, 383 are alive and over 16 years old at the last check. Thus, the 23 described in this case-series represent 6% of those with a similar child-bearing age. It is worth noting that 5 had more than one child. In spite of the prolonged history of HIV-1 infection and of targeted therapies, the good quality of life and a longer life expectancy presumably allowed these women to live motherhood with fewer distressing concerns. The low probability of HIV-1 transmission to the offspring is an additional important factor supporting such women having children. We have no documentation about the possible birth control methods adopted by these women, or whether these pregnancies were planned. However, the median age of our parturients was rather lower than the 32.3 years observed in the general Italian population [16]. This low median age at delivery is consistent with other reports [3,5,6,10], and, perhaps, mirrors the fear that the chronic disease could deprive them of the special female role of motherhood. This growing desire of motherhood among seropositive women clearly emerges from our Register, where the number of HIV-1 perinatally-exposed children is around 350–400 per year, with an increasing multiparity rate, reaching 25% in recent years (data not shown).

In this scenario, the management of HIV-1 perinatally-infected pregnant women and their children will be an important challenge for clinicians in the near future. A crucial aspect will be the choice of the best ART regimen to prevent MTCT. None of our mothers was perinatally exposed to ART drugs, as they were born before the ACTG 076 protocol [17,18]. However, the majority received ART therapy during childhood and experienced several sub-therapeutic regimens. Although resistance data were not available, these conditions are well known to favour the development of drug resistant viruses, with a consequent possible higher risk of MTCT, a phenomenon that fortunately does not emerge from the available data. As far as AZT is concerned, it is worth noting that over half of our mothers started AZT as a monotherapy during childhood, then shifted to a dual therapy including AZT, continuing with such combinations for several years. Six of these 14 women continued to receive AZT also during pregnancy, as did all their children as a prophylaxis, apparently with success, since the majority of the mothers had undetectable viral loads at delivery and no child acquired the infection. This casts doubts on the suggested exclusion of AZT during pregnancy if there had been a prolonged monotherapy during childhood [10]. Indeed, in a recent case series the role of intrapartum intravenous AZT for the prevention of MTCT in women with virological failure has been stressed [19]. AZT may be effective in the prevention of MTCT through other mechanisms besides its direct antiviral effect [18,20].

The possible impact of a prolonged ART therapy on maternal and child health is a further important aspect. Even in this context, our results are reassuring. No congenital abnormalities were noticed, including the child exposed to EFV in the first 5 weeks of gestation [21,22]. Since maternal and neonatal complications due to ART drugs do not seem to be higher in perinatally-infected women, indications should not differ from those commonly recommended in seropositive mothers, for instance HAART should start as soon as possible [15], while stopping ART during pregnancy should be discouraged [12]. In fact, fearing a possible teratogenicity, 3 women discontinued ART treatment during the first trimester of pregnancy and their viral load was detectable at delivery. On the other hand, the experience of several therapeutic regimens during childhood and adolescence will presumably lead to the use of new antiretroviral drugs during pregnancy, such as integrase inhibitors, the impact of which on pregnant women and their foetuses still needs to be elucidated.

Conclusions

The outcome of second-generation HIV-1 exposed infants seems favourable. In spite of a long course of maternal infection, multiple ART regimens, and a possible development of drug-resistant viral strains, MTCT continues to be efficiently controlled by the commonly adopted preventive strategies, even though an adequate surveillance of pregnancy among this unique population is highly recommended.

Competing interests

The Italian Register for HIV Infection in Children was funded by the Istituto Superiore di Sanità, Rome, Italy, and the Paediatric European Network for Treatment of AIDS (PENTA) Foundation, Padua, Italy. The authors declare that they have no competing interests.

Authors’ contributions

All Authors and Co-Authors contributed equally to the study design, acquisition of women and children information and interpretation of data. CC, CG and PAT drafted the manuscript, while MdM, LG, EC, CG, WB, OG, SE, SB critically revised it for its intellectual content. All Authors and Co-Authors accepted the final version of the manuscript.

Authors’ information

Co-Authors: Giacomo Faldella (Bologna), Raffaele Badolato, Chiara Monfredini (Brescia), Cristina Gotta (Genoa), Vania Giacomet (Milan), Monica Cellini (Modena), Osvalda Rampon (Padua), Maura Agnese (Naples), Piero Valentini (Rome), Carlo Scolfaro, Silvia Garazzino (Turin), Antonio Mazza (Trento).

Pre-publication history

The pre-publication history for this paper can be accessed here:

http://www.biomedcentral.com/1471-2334/14/277/prepub

Contributor Information

Carmelina Calitri, Email: carmelina_calitri@libero.it.

Clara Gabiano, Email: clara.gabiano@unito.it.

Luisa Galli, Email: luisa.galli@unifi.it.

Elena Chiappini, Email: elena.chiappini@unifi.it.

Carlo Giaquinto, Email: carlog@pediatria.unipd.it.

Wilma Buffolano, Email: wilma@unina.it.

Orazio Genovese, Email: hor6505@yahoo.com.

Susanna Esposito, Email: susanna.esposito@unimi.it.

Stefania Bernardi, Email: s.bernardi@opbg.net.

Maurizio De Martino, Email: maurizio.demartino@unifi.it.

Pier-Angelo Tovo, Email: pierangelo.tovo@unito.it.

Acknowledgements

All principal investigators and sites who participate in the ITLR have been previously published [1] and are listed below. The Authors are grateful to Andrew Martin Garvey for editorial assistance and to Federica Messina for data management.

The "Italian Register for HIV infection in children" principal investigators by site are: Patrizia Osimani (Ancona), Domenico Larovere (Bari), Maurizio Ruggeri (Bergamo), Andrea Pession, Giacomo Faldella (Bologna), Francesca Capra, Sara Pulcini, Valentina Zattoni (Brescia), Maurizio Dedoni (Cagliari), Antonia Aliffi (Catania), Elisa Anastasio (Catanzaro), Elisa Fiumana (Ferrara), Paola Gervaso, Carlotta Montagnani (Florence), Antonio Di Biagio, Laura Ambra Nicolini, Laura De Hoffer, Maria Sole Acutis, Elisabetta Bondi (Genoa), Paola Erba, Valentina Fabiano, Giulia Ramponi, Filippo Salvini, Rita Lipreri, Susanna Esposito, Anna Plebani, Claudia Tagliabue (Milan), Francesca Giubbarelli (Modena), Emanuele Nicastro, Andrea Lo Vecchio, Wilma Buffolano, Maura Agnese (Naples), Amelia Romano (Palermo), Carlo Giaquinto, Osvalda Rampon, Martina Pennazzato (Padua), Rita Consolini (Pisa), Icilio Dodi (Parma), Anna Maccabruni (Pavia), Orazio Genovese, Paolo Palma, Giuseppe Pontrelli, Hyppolite Tchidjou (Rome), Paolina Olmeo (Sassari), Antonio Mazza (Trento), Erika Silvestro, Silvia Virano (Turin), Vincenzo Portelli (Trapani), Marco Rabusin (Trieste), Antonio Pellegatta (Varese).

References

  1. De Martino M, Tovo PA, Balducci M, Galli L, Gabiano C, Rezza G, Pezzotti P. Reduction in mortality with availability of antiretroviral therapy for children with perinatal HIV-1 infection. Italian Register for HIV infection in children and the Italian National AIDS Registry. JAMA. 2000;14:190–197. doi: 10.1001/jama.284.2.190. [DOI] [PubMed] [Google Scholar]
  2. Gortmaker SL, Hughes M, Cervia J, Brady M, Johnson GM, Seage GR III, Song LY, Dankner WM, Oleske JM. Pediatric AIDS Clinical Trials Group Protocol 219 Team. Effect of combination therapy including protease inhibitors on mortality among children and adolescents infected with HIV-1. N Engl J Med. 2001;14:1522–1528. doi: 10.1056/NEJMoa011157. [DOI] [PubMed] [Google Scholar]
  3. Thorne C, Townsend CL, Peckham CS, Newell ML, Tookey PA. Pregnancies in young women with vertically acquired HIV infection in Europe. AIDS. 2007;14:2552–2556. doi: 10.1097/QAD.0b013e3282f08b5f. [DOI] [PubMed] [Google Scholar]
  4. Elgalib A, Hegazi A, Samarawickrama A, Roedling S, Tariq S, Draeger E, Hemelaar J, Rathnayaka T, Azwa A, Hawkins D, Edwards S, Perez K, Russell J, Wood C, Poulton M, Shah R, Noble H, Rodgers M, Taylor GP, Anderson J, de Ruiter A. Pregnancy in HIV-infected teenagers in London. HIV Med. 2011;14:118–123. doi: 10.1111/j.1468-1293.2010.00878.x. [DOI] [PubMed] [Google Scholar]
  5. Centers for Disease Control and Prevention. Pregnancy in perinatally HIV-infected adolescents and young adults--Puerto Rico, 2002. MMWR Morb Mortal Wkly Rep. 2003;14:149–151. [PubMed] [Google Scholar]
  6. Chibber R, Khurranna A. Birth outcomes in perinatally HIV-infected adolescents and young adults in Manipur, India: a new frontier. Arch Gynecol Obstet. 2005;14:127–131. doi: 10.1007/s00404-003-0564-z. [DOI] [PubMed] [Google Scholar]
  7. Crane S, Sullivan M, Feingold M, Kaufman GE. Successful pregnancy in an adolescent with perinatally acquired human immunodeficiency virus. Obstet Gynecol. 1998;14:711. doi: 10.1016/S0029-7844(98)00292-0. [DOI] [PubMed] [Google Scholar]
  8. Levine AB, Aaron E, Foster J. Pregnancy in perinatally HIV-infected adolescents. J Adolesc Health. 2006;14:765–768. doi: 10.1016/j.jadohealth.2005.06.010. [DOI] [PubMed] [Google Scholar]
  9. Brogly SB, Watts DH, Ylitalo N, Franco EL, Seage GR 3rd, Oleske J, Eagle M, Van Dyke R. Reproductive health of adolescent girls perinatally infected with HIV. Am J Public Health. 2007;14:1047–1052. doi: 10.2105/AJPH.2005.071910. [DOI] [PMC free article] [PubMed] [Google Scholar]
  10. Williams SF, Keane-Tarchichi MH, Bettica L, Dieudonne A, Bardeguez AD. Pregnancy outcomes in young women with perinatally acquired human immunodeficiency virus-1. Am J Obstet Gynecol. 2009;14:149.e1–5. doi: 10.1016/j.ajog.2008.08.020. [DOI] [PubMed] [Google Scholar]
  11. Cruz MLS, Cardoso CA, João EC, Gomes IM, Abreu TF, Oliveira RH, Machado ES, Dias IR, Rubini NM, Succi RM. Pregnancy in HIV vertically infected adolescents and young women: a new generation of HIV-exposed infants. AIDS. 2010;14:2727–2731. doi: 10.1097/QAD.0b013e32833e50d4. [DOI] [PubMed] [Google Scholar]
  12. Galli L, Puliti D, Chiappini E, Gabiano C, Ferraris G, Mignone F, Viganò A, Giaquinto C, Genovese O, Anzidei G, Badolato R, Buffolano W, Maccabruni A, Salvini F, Cellini M, Ruggeri M, Manzionna M, Bernardi S, Tovo P, de Martino M. Italian Register for HIV Infection in Children. Is the interruption of antiretroviral treatment during pregnancy an additional major risk factor for mother-to-child transmission of HIV type 1? Clin Infect Dis. 2009;14:1310–1317. doi: 10.1086/597774. [DOI] [PubMed] [Google Scholar]
  13. Bertino E, Spada E, Occhi L, Coscia A, Giuliani F, Gagliardi L, Gilli G, Bona G, Fabris C, De Curtis M, Milani S. Neonatal anthropometric charts: the Italian neonatal study compared with other European studies. J Pediatr Gastroenterol Nutr. 2010;14:353–361. doi: 10.1097/MPG.0b013e3181da213e. [DOI] [PubMed] [Google Scholar]
  14. Italian Register for Human Immunodeficiency Virus Infection in Children. Determinants of mother-to-infant human immunodeficiency virus 1 transmission before and after the introduction of zidovudine prophylaxis. Arch Pediatr Adolesc Med. 2002;14:915–921. doi: 10.1001/archpedi.156.9.915. [DOI] [PubMed] [Google Scholar]
  15. Centers for Disease Control and Prevention. Recommendations for Use of Antiretroviral Drugs in Pregnant HIV-1-Infected Women for Maternal Health and Interventions to reduce Perinatal HIV Transmission in the United States. 2012. Available at: http://aidsinfo.nih.gov/guidelines.
  16. Italian Department of Health. Certificato di assistenza al parto (CeDAP) Analisi dell’evento nascita - Anno2009. Available at: http://www.salute.gov.it/imgs/C_17_pubblicazioni_1731_allegato.pdf.
  17. Centers for Disease Control and Prevention. Zidovudine for the prevention of HIV transmission from mother to infant. MMWR Morb Mortal Wkly Rep. 1994;14:285–287. [PubMed] [Google Scholar]
  18. Sperling RS, Shapiro DE, Coombs RW, Todd JA, Herman SA, McSherry GD, O’Sullivan MJ, Van Dyke RB, Jimenez E, Rouzioux C, Flynn PM, Sullivan JL. Maternal viral load, zidovudine treatment, and the risk of transmission of human immunodeficiency virus type 1 from mother to infant. Pediatric AIDS Clinical Trials Group Protocol 076 Study Group. N Engl J Med. 1996;14:1621–1629. doi: 10.1056/NEJM199611283352201. [DOI] [PubMed] [Google Scholar]
  19. Briand N, Warszawski J, Mandelbrot L, Dollfus C, Pannier E, Cravello L, Nguyen R, Matheron I, Winer N, Tubiana R, Rouzioux C, Faye A, Blanche S. ANRS-EPF CO1-CO11 Study Group. Is intrapartum intravenous zidovudine for prevention of mother-to-child HIV-1 transmission still useful in the combination antiretroviral therapy era? Clin Infect Dis. 2013;14:903–914. doi: 10.1093/cid/cit374. [DOI] [PubMed] [Google Scholar]
  20. Bassetti D, Cargnel A. Genotypic resistance tests for the management of the HIV-infected pregnant woman. Scand J Infect Dis Suppl. 2003;14:70–74. [PubMed] [Google Scholar]
  21. Ford N, Mofenson L, Kranzer K, Medu L, Frigati L, Mills EJ, Calmy A. Safety of efavirenz in first-trimester of pregnancy: a systematic review and meta-analysis of outcomes from observational cohorts. AIDS. 2010;14:1461–1470. doi: 10.1097/QAD.0b013e32833a2a14. [DOI] [PubMed] [Google Scholar]
  22. Ford N, Calmy A, Mofenson L. Safety of efavirenz in the first trimester of pregnancy: an updated systematic review and meta-analysis. AIDS. 2011;14:2301–2304. doi: 10.1097/QAD.0b013e32834cdb71. [DOI] [PubMed] [Google Scholar]

Articles from BMC Infectious Diseases are provided here courtesy of BMC

RESOURCES