1 / 19

HIV in Pregnancy

HIV in Pregnancy. Max Brinsmead PhD FRANZCOG May 2011. Human Immunodeficiency Virus. HIV is a Lentivirus A member of the Retrovirus family Infects helper T cells (CD4), macrophages & mucosal dendritic cells Depletes CD4 numbers & thereby cell-mediated immunity

urban
Download Presentation

HIV in Pregnancy

An Image/Link below is provided (as is) to download presentation Download Policy: Content on the Website is provided to you AS IS for your information and personal use and may not be sold / licensed / shared on other websites without getting consent from its author. Content is provided to you AS IS for your information and personal use only. Download presentation by click this link. While downloading, if for some reason you are not able to download a presentation, the publisher may have deleted the file from their server. During download, if you can't get a presentation, the file might be deleted by the publisher.

E N D

Presentation Transcript


  1. HIV in Pregnancy Max Brinsmead PhD FRANZCOG May 2011

  2. Human Immunodeficiency Virus • HIV is a Lentivirus • A member of the Retrovirus family • Infects helper T cells (CD4), macrophages & mucosal dendritic cells • Depletes CD4 numbers & thereby cell-mediated immunity • Opportunistic infections and/or tumours then begin • This is then known as AIDS • Which untreated is fatal within 12m

  3. HIV Infection • Two subtypes of the virus • HIV1 - global • HIV2 – mostly limited to West Africa • This virus is transmitted by… • Blood and blood products • Tissue • Semen • Vaginal fluids • Transplacental • Breast milk • Although found in tears, saliva and urine it is not transmitted by these fluids

  4. After exposure to HIV • Incubation period of 2 – 4 weeks • Then an acute CMV-like illness • Fever • Lymphadenopathy • Pharyngitis • Myalgia & malaise • Lasts about 28 days • Median seroconversion time is 22 days • Then Latent Phase of 2 – 20 years depends on: • Host response • Viral factors • Environmental factors • Treatment (if any) • Untreated →typically AIDS within 10 years

  5. HIV transmission risk • Female to male 0.04% rate per coital act • Male to female 2-fold higher • But 4 -10fold higher in developing countries • Receptive anal coitus 1.7% rate per act • Condoms reduce the risk by 85% • Circumcision reduces ♀→♂ rate by 50% • Needlestick 0.3% rate per injury • Maternal to Child Transmission (MTCT) with pregnancy, birth & breastfeeding 25 – 48% • >400,000 new cases per year worldwide

  6. HIV Diagnosis • Screen by ELISA (very sensitive) • Retest those that are positive in duplicate • The confirmatory test is Western Blot (WB) • or IFA (less commonly done) • Inconclusive WB – repeat after 28 days • Risk of false positive in this 2-step procedure is <1:10,000 • Disease activity is measured by CD4 count • And less commonly by viral load (RNA or DNA) as measured by PCR or TMA • P24 antigen testing is for the virus itself – has very low sensitivity

  7. HIV Treatment • Typically only commences when CD4 counts fall below 350 • Optimally comprises triple therapy with HAART • HAART = Highly active antiretroviral therapy • This prolongs latent period by 20 – 50 years • Successful treatment reduces detectable virus to zero over 4 - 6 months • However, this is achieved only 50% of the time because of: • Side effects • Non compliance for financial, psychological or other reasons • Viral drug resistance • In resource-rich settings HAART may start earlier

  8. WHO Staging (2005) >15 yrs of Age • Clinical stage 1 • Asymptomatic • Persistent generalized lymphadenopathy • Clinical stage 2 • Weight loss (<10% of presumed or measured body weight) • Recurrent respiratory tract infections (such as sinusitis, bronchitis, otitis media, pharyngitis) • Herpes zoster • Recurrent oral ulcerations • Papularpruritic eruptions • Angular cheilitis • Seborrhoeic dermatitis • Fungal finger nail infections

  9. WHO Staging (2005) >15 yrs of Age • Clinical stage 3 • Unexplained chronic diarrhoea >1 month • Unexplained persistent fever >1 month) • Weight loss (>10% of presumed or measured body weight) • Oral candidiasis • Oral hairy leukoplakia • Pulmonary TB • Severe infections e.g. pneumonia, empyema, meningitis, bacteraemia, pyomyositis, bone or joint infection • Acute necrotizing ulcerative stomatitis, gingivitis or periodontitis

  10. WHO Staging (2005) >15 yrs of Age • Clinical Stage 4 • HIV wasting syndrome • Pneumocystis pneumonia • Recurrent pneumonia • Herpes simplex >1 month • Oesophageal candidiasis • Extrapulmonary TB • Kaposi’s sarcoma • CNS toxoplasmosis • HIV encephalopathy

  11. WHO Staging (2005) >15 yrs of Age • Stage 4 (with additional tests) • Extrapulmonarycryptococcosis • Disseminated non-TB mycobacteria • Progressive multifocal leukoencephalopathy • Candida of trachea, bronchi or lungs • Cryptosporidiosis • Isosporiasis • Visceral herpes simplex infection • CMV retinitis or any organ other than liver, spleen or lymph nodes) • Any disseminated mycosis e.g. histoplasmosis, coccidiomycosis, penicilliosis • Recurrent non-typhoidal salmonella • Lymphoma (cerebral or B cell non-Hodgkin) • Cervical carcinoma • Visceral Leishmaniasis

  12. HIV Treatment in Resource-Poor Areas • Clinically advanced HIV disease • WHO Stage 4 irrespective of the CD4 cell count • WHO Stage 3 + consider using CD4 < 350 to assist decision making • WHO Stage 2 or 1 with CD4 counts < 200

  13. Effects of HIV on Pregnancy • Risk of maternal death is increased 6-fold • Concurrent infections including TB • All obstetric causes • Increased risk of poor obstetric outcome • Miscarriage • Stillbirth • Pre term birth • IUGR • Mother to Child transmission (MTC) of HIV • Is the most common means of HIV transmission in the world • Risk is 25 – 50%

  14. Risk Factors for Mother to Child Transmission • Primary HIV infection • Repeat testing of high risk individuals may be required • Concurrent infections including TB and STI • High maternal viral load and low CD4 counts • Prolonged rupture of membranes • Vaginal delivery • Fetal trauma during delivery • Breast feeding • High viral load in breast milk • Mastitis

  15. HIV Mother to Child Transmission • 80% occurs during labour • Can be reduced by 50% Caesarean section before membranes rupture • But only used where CS is safe in the short and long term • And viral load is >1,000 ml/plasma • Next best option is a single dose of NVP at least 2 hours before delivery. Follow up with AZT + 3TC for one week • Give the baby one shot of NVP when born + AZT for one week • Risk of MTC is then approx. 5% • If mother receives triple therapy from <28w, has elective CS & does not breast feed MTCT is 1-2%

  16. Nevirapine Resistance • Single dose Nevirapine (NVP) before delivery is widely used in resource-poor settings to prevent MCT of HIV • But this induces NVP resistance in 12 – 14% of mothers AND babies • So double or triple therapy is preferred • If you can afford it

  17. Cochrane on HIV in Pregnancy • All adults with HIV and CD4 count <350 require HAART for life • The best predictor of maternal health and MTCT is plasma viral load. Aim for <500/ml • Risk of teratogenesis in the 1st trimester to be weighed against maternal need for HAART • WHO guidelines now assume benefits exceed risk • Regimens with LPV have an increased risk of prematurity • Regimens with NVP have increased rates of adverse maternal effects • Best regimen is therefore AZT/3TC/ABC followed by dual or triple therapy especially if breastfeeding • MTCT rate after vaginal delivery is then ≈ 12%

  18. Current WHO Guidelines • All HIV patients to begin HAART asap • Continue right through VAGINAL DELIVERY • Tail off non-eligible mothers from therapy after they have stopped breast feeding AND • Give the infant oral NVP whilst ever mother is breastfeeding plus one week (up to 12 months) • Mothers eligible to continue triple therapy to continue whilst breast feeding PLUS • Give the neonate 6 weeks of AZT and NVP for as long as the mother is breast feeding • It is hoped that MTC will be 1-2%

  19. HOWEVER… All of this presupposes that… All pregnant women will commence antenatal care at <14 weeks gestation All women will have a HIV test High risk women will have a second HIV test There are medical resources to provide optimal therapy All HIV-positive women will take the therapy and give it to their babies as prescribed

More Related