S E P T E M B E R  2 0 1 0                           T H E  S O U T H E R N  A F R I C A N  J O U R N A L  O F  H I V  M E D I C I N E                                                  

Effective prevention of mother-to-child transmission 
(PMTCT) strategies are known to reduce the incidence 
of paediatric HIV infection.1 A small non-governmental 
project at McCord Hospital in Durban, KwaZulu-Natal, 
with access to highly active antiretroviral therapy 
(HAART), reported vertical transmission of 2.9%. 
The authors of that paper also reported results of 
two studies in the public sector, in 2002 and 2006, 
respectively, where transmission rates of 8.7% and 
20.8% were achieved with a PMTCT drug regimen 
comprising single-dose nevirapine (sdNVP).2 These 
were in Gauteng and KwaZulu-Natal respectively, 
while in the Western Cape in 2003 a rate of 8.8% was 
recorded for women given dual therapy of zidovudine 
(ZDV) from 34 weeks and sdNVP.3 

In the private sector, many patients belong to medical 
scheme-funded disease management programmes, 
such as Aid for AIDS (AfA). PMTCT guidelines for 
developed countries, where HIV-infected newborns are 
becoming uncommon, are followed.1,4 The programme 
comprises prenatal HIV-1 counselling and testing, and 
HAART (irrespective of CD4 count) from the second 
trimester onwards, unless the mother is already on 
antiretrovirals or fulfils the criteria for starting HAART 
immediately. Elective caesarean section, together with 
intrapartum intravenous ZDV, is offered and ZDV is 
given to the neonate. Formula feeding is supplied for 6 
months and breastfeeding is avoided.

While many private practitioners follow AfA guidelines, 
they may use different regimens, depending on cost 
considerations. The present study aimed to investigate 

the outcome of infants born to HIV-positive mothers 
managed in a group of private paediatric practices in 
central Durban, KwaZulu-Natal.

METHODS

Ethical approval for this retrospective chart review 
was obtained from the Biomedical Research Ethics 
Committee of the Nelson R Mandela School of 
Medicine (Reference number BEO47/47). Of the 20 
paediatricians in the Durban Central region, 4 (20%) 
did not respond. All charts of HIV-exposed infants 
born between January 2004 and June 2005, from 
the 8 paediatricians who agreed to participate, were 
included. Data were collected by means of previously 
piloted questionnaires.

RESULTS

One hundred and one charts were available, of which 
50 came from a single practice (which is an HIV referral 
centre). The balance was contributed approximately 
equally by the remaining practitioners. 

One hundred and one infants (one set of twins) were 
delivered to 100 black African women, 93 by caesarean 
section. Fifty infants were boys, 20 were low birth 
weight, 2 were large for gestational age and 79 were 
appropriate for gestational age. Ninety-seven mothers 
were medical scheme beneficiaries (86 contracted to 
AfA). The mean age was 30 (range 18 - 44) years and 
mean parity was 1 child (range 1 - 4). Presentation 
and antenatal care initiation were in the first, second 

PREVENTION OF MOTHER-TO-CHILD 
TRANSMISSION OUTCOMES IN THE 

PRIVATE SECTOR IN CENTRAL DURBAN

o r i g i n a l  a r t i c l e

Shakira M Cassim, MB ChB, DCH (SA) FCPaed (SA), MPH, Dip HIV Man (SA)
Julia H Botha, BPharm, PhD

Department of Therapeutics and Medicines Management, Nelson R Mandela School of Medicine, Durban

The prevention of mother-to-child transmission (PMTCT) programme in the central region of Ethekweni Metro, 
KwaZulu-Natal (Durban central area), was investigated. Data for all HIV-exposed infants from eight private 
paediatric practices seen between January 2004 and June 2005 were reviewed retrospectively. One hundred 
and one black African infants were born to 100 HIV-positive women of average age 30 years. Median viral loads 
and CD4 counts were 11 391 copies/ml and 426 cells/μl, respectively. Eighty-six women received HAART and 5 
had no prophylaxis. Of the 92 infants tested, 2 were HIV positive, giving a transmission rate of 2.2%. Both their 
mothers had received suboptimal prophylaxis, and if they are excluded, the transmission rate falls to less than 
1%, a rate consistent with those in the developed world.

6



T H E  S O U T H E R N  A F R I C A N  J O U R N A L  O F  H I V  M E D I C I N E                          S E P T E M B E R  2 0 1 0

and third trimesters for 40%, 34% and 26% of mothers, 
respectively. HIV infection had been diagnosed in the 
current pregnancy in the majority (75%) of cases, and 
the rest already knew their status.

Viral load and CD4 count measurements were recorded 
for 86 and 91 women, respectively. The median CD4 
count was 426 (intraquartile range (IQR) 244 - 613) 
cells/μl. Only 13% of the women had CD4 counts 
less than 200 cells/μl. The median viral load at first 
presentation was 3.97 (IQR 1.6 - 5.8) logs or 11 391 
(IQR 2 013 - 41 502) copies/ml. 

Eighty-six women (86.0%) received HAART. This 
comprised ZDV and lamivudine (3TC), either together 
with lopinavir/ritonavir (if the CD4 count was >250) 
or together with NVP if the CD4 count was <250. The 
regimen also included intrapartum intravenous ZDV. 
Nine women did not receive HAART; 7 received only 
intrapartum intravenous ZDV, 1 had only intrapartum 
NVP, and 1 had dual therapy with ZDV/3TC. Treatment 
was initiated at less than 28 weeks in 32 women and 
between 28 and 34 weeks in 41 women. Five women 
received no prophylaxis because they presented for 
antenatal care very late in the third trimester.

All infants were formula fed and received ZDV for 6 
weeks. Haemoglobin (Hb) measurements in 98 patients 
revealed 18 (4 preterm) with anaemia. Seventy-nine 
infants received PCP prophylaxis. There were 18 preterm 
infants, half of whom were born to women with low CD4 
counts who received NVP as part of their HAART. Five 
and 3 of the premature infants were born to mothers 
who had received protease inhibitors and no prophylaxis, 
respectively. One of the latter 3 seroconverted.

Eight infants defaulted follow-up and 1 died (of unknown 
cause) at 5 weeks before testing was possible. Ninety-
two infants were tested, 61 of them by polymerase 
chain reaction (PCR) at 6 weeks. Fifty-six were tested 
by enzyme-linked immunosorbent assay (ELISA) at 18 
months (some of whom had already had a first PCR). 
Two infants were diagnosed positive, and their details 
are set out in Table I.

DISCUSSION

Although our transmission rate of 2.2% appears 
better than the 2.9% from the McCord experience, 
the proportions of women in that group with low CD4 
counts and receiving HAART were double and half, 
respectively. Our rate was not as good as the situation 
that pertains in the USA and Europe, where HIV-infected 
newborns are becoming uncommon, but is close to the 

1 - 2% transmission expected for women from socio-
economically advantaged areas in Africa who can safely 
formula feed.1

 
The mothers of both positive infants had suboptimal 
PMTCT, and if these women are excluded the transmission 
rate falls to less than 1%. In fact, in those women who 
were fully compliant there was no transmission.

One of the 2 mothers had been diagnosed 2 years 
before the pregnancy and presented for antenatal care 
but was not on medical aid and could not afford HAART. 
It had been planned to initiate HAART at 34 weeks, but 
she went into labour at 33 weeks. The other mother 
was diagnosed early in the current pregnancy but did 
not return for results, so HAART was initiated only 5 
days before delivery. Non-adherence is a risk factor in 
perinatal transmission, but it is a problem with which 
even a developed country like the UK is grappling.5

Our study has confirmed the success of an appropriate 
PMTCT programme and the importance of prophylaxis 
and adhering to the protocol.

reFerenceS
1.  Coovadia HM. Perspectives on paediatric HIV/AIDS: Prevention of mother to child 

transmission of HIV. Current Science 2008; 95(9): 1133-1149.
2.  Geddes R, Knight S, Reid S, Giddy J, Esterhuizen T, Roberts C. Prevention of 

mother-to-child transmission of HIV programme: low vertical transmission in 
KwaZulu-Natal, South Africa. S Afr Med J 2008; 98: 458-462.

3.  Draper B, Abdullah F. A review of the prevention of mother-to-child transmission 
program of the Western Cape provincial government 2003-2004. S Afr Med J 
2008; 98: 431-434.

4.  Regensberg L, Makiwane M. AfA Clinical Guidelines. 7th ed. Pinelands: Aid for 
AIDS; 2009. http://www.aidforaids.co.za/EX_Medscheme_VS07/Documents/
AFA/Guidelines_book_Final.pdf (accessed 30 May 2009). 

5.  Kingston MA, Letham CJ, McQuillan O. Adherence to antiretroviral therapy in 
pregnancy. Int J STD AIDS 2007; 18(11): 787-789.

7

 Infant 1 Infant 2
Birth weight (kg) 2.2 3.0
Gestational age  33 38 
(wks) 
Health at birth Congenital  Well 
 pneumonia,  
 anaemia 
Treatment ZDV for 6 weeks ZDV for 6 weeks
 Mother 1 Mother 2
Age (yrs) 28 37
Mode of delivery Caesarean section Caesarean section
Diagnosis of HIV 2 - 3 years earlier During current  
  pregnancy 
ART prophylaxis None  HAART initiated  

5 days before  
delivery

Intrapartum IV ZDV Yes Yes
Viral load at  Not recorded 50 000 
delivery   copies/ml
CD4 count at delivery Not recorded 327 cells/μl

taBle i. DetailS oF tHe 2 HiV-PoSitiVe inFantS