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1
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2
Perinatal Transmission Of Infectious Disease
Oormila P. Kovilam, M.D. University of
Cincinnati Department of Obstetrics
Gynecology Cincinnati STD/HIV Prevention Training
Center
3
World wide prevalence

• 39 million ww, 50 women.

• gt 10 million
• gt 50 ?
• 25 unaware
• 300 newborns/yr.
• No decline in rate

4
HIV Pregnancy

• Initial 5 cases of PCP in men (1981)
• 25 yrs. later, AIDS in ? 7 ? 27
• 7 10,000 babies born/yr. to ve ?
• 2 3,000 will be ve
• Can ? to lt 500 by universal screening

5

• ? testing/
• 3 phase therapy
• ? to 2

6
MAGNITUDE OF MTCT

• Trend is rising
• Most tragic consequence of HIV epidemic
• 650,000 infected/day ww.
• 75 MTCT
• Detrimental tochild survival program

7
WHY DOES PERINATAL TRANSMISSION STILL OCCUR?

• 25 unaware
• 78 AIDS in women of color
• 1/9 no prenatal care
• No care until labor
• Test ? Treatment delay
• Compliance/Resistance

8
Prevalence of DZ screened for in newborns

• MSU 1 175,000
• Homocystinuria 1100,000
• Galactosemia 1 60,000
• PKU 114,000
• Tyrosinemia 1 300,000
• Hypothyroidism 14000
• Perinatal HIV 11500

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WHY A NEW INITIATIVE

• HIV at its highest
• Availability of a simple, rapid HIV test
• 40 of infected newborn born to unaware pregnant
  women
• 95 AZT/ 01 combination Rx
• 03 no child to be born with unknown status

LD a 48 hr Window
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SCREENING

• CDC screening
• Prenatal opt out
• LD rapid testing
• Post-natal Rapid testing to status unknown

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Rapid testing

• Point of care test Rx ? time of
  unawareness to awareness
• 100 vs. 84notification
• Critical in ICU, surgical obstetric setting
• UNO WHO recommend rapid testing instant
  notification of result

12
Turn around Time

• Point of care 45 mts 0 .5-2.5 hrs (LD)
• Laboratory 210 mts 1.6-16 hrs
• Mmwr 5236 2003

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RAPID TEST
Mother infant rapid intervention at delivery
(MIRIAD) 70 to ? - 5 hrs to Rx
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FDA APPROVED RAPID TESTS

• Sensitivity Specificity
• (95 C.I.) (95 C.I.)
• OraQuick Advance
• whole blood 99.6
  100
• oral fluid 99.3
  99.8
• Uni-Gold Recombigen
• whole blood 100
  99.7
• serum/plasma 100
  99.8
• Reveal g2
• Multispot HIV-1/ HIV2

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Rapid Protocol Team

• Obstetrician Epidemiologist
  Laboratory
• Pediatrician
• Health educator

• Infectious disease
• Social worker
• Public Health Nursing

16
Third Trimester Testing

• Before 36 wks.
• History of STD
• Multiple partners
• Illicit drugs
• Symptoms/ signs of seroconversion

17
TRANSMISSION - TIMING

• In utero 25 - 40 of cases
• Intrapartum 60 - 75 of cases
• Addition risk with breastfeeding
• 14 ? risk with established infection
• 29 ? risk with primary infection
• most transmission during intrapartum period

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DETERMINANTS OF TRANSMISSION

• Maternal disease stage
• Advanced stage higher transmission
• AIDS
• Lower CD4 counts
• Maternal p24 antigenemia
• High plasma RNA levels

• Obstetrical Factors
• Length of PROM
• Infection
• Vaginal delivery
• Invasive procedures
• Infant Factors
• Prematurity
• Susceptibility

19
Vertical Transmission

• In Utero lt 10
• Peripartum 40 70
• Breast feeding 0.5 /m risk
• Most important factor Viral load

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Chorio in utero
22
Chorio Placenta
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Acute Chorioamnionitis
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ABRUPTIO PLACENTA

• Perinatal Transmission not all related to viral
  load

25
HSV - FEMALE
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Trichomonas Vaginalis
27
Cervical Intraepithelial Neoplasia
28
TWIN GESTATION
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MULTIPLE GESTATION
Most vulnerable closest to cervix
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Short Cervix with funneling
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Chemical structure of Zidovudine
AZT (Zidovudine)
32
ACTG 076

• Early ARV Rx
• 94 ACTG 076 AZT ? MTCT
• HIV CD4 gt 200 (N477)
• N180 N185

ZDV 100mg x 5/day Placebo 2 mg/kg loading
IV 1 mg/kg till delivery 2 mg/kg q 6 hr.
infant thru 6 wks. HIV 13 HIV 40
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Results of ACTG
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Perinatal Transmission through the years

• Without ARV 16 25 (WITS 93)
• Newborn ve
• A2T 7.6 (ACTG 076 94)
• A2T C/S 2 (06)
• HAART C/S 1 (06)

MTCT
35
VL in Genital Secretions MTCT (Thailand)
Chuachoowong et al. JID 2000(181) p. 105
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PREGNANCY CONCERNS

• Physiological changes
• Less aggressive use of therapy
• Treatment to ? MTCT resistant strains
• Less compliance

37
Unique pharmacokinetics

• Placenta with increase flow
• Transport of drugs
• Compartmentalization of drugs
• Biotransformation of drugs by fetus placenta
• Elimination of drugs by fetus

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Effect of drugs of fetus/newborn

• Teratogenicity
• Mutagenicity
• Carcinogenicity
• Hemolytic anemia
• PK toxicity of transplacental drugs
• Barkers Hypothesis

39
Perinatal Guidelines

• 94 in response to ACTG 076
• Working group established inDecember 99

40
Care guidelines

• Define HIV stage/CD4, viral load
• Concurrent Risk factors
• Plan care for pregnancy, delivery infant
• Comprehensive care HAART
• Compliance/Risk for resistance

41
Anti retroviral therapy

• Site of action
• lt insert picturegt

42
HAART in pregnancy

• NRTI - Nucleoside RTI
• NNRTI - Non Nucleoside RTI
• PI - Protease Inhibitors

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Counsel Woman

• Importance of adherence to care
• Important to take every pill every day
• Seek care of experienced OBS/ID team
• Obtain all laboratory tests on schedule
• Immediate follow up for new symptoms

44
Changing ART during Pregnancy

• Poor CD4 response
• Drugs with potential teratogenicity
• Poor viral load response
• Poor adherence to regimen
• Evidence of viral resistance

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PRENATAL DIAGNOSIS
46
INTRAPARTUM

• 1991 European Collaborative study
• 1993 Le Zuriages et al
• 1994 McIntosh et al
• 1994 McIntosh
• 1995 Duliege I of twin effected more
• 1995 Minkoff increase with PROM

47
PERINATAL TRANSMISSION
Confidence Interval
48
Comparison of Regimens
49
HIV transmission Mode of Delivery
50
ROLE OF C/S

• Amsley,Momif 1974 Protective effect of
  HIV
• Lee 1988 Decrease Hep B
• Shah 1986 Decrease HIV
• Fr Perinatal 1998 Elective (.8)
  (n87)
• Emergency
  (11.4)
• Vaginal (6.6)
  P0.02
• Kind 1998 Swiss
  neonatal HIV study
• Gibbs 2000 Decrease Hep C
  transmission
• 4-hour rule guiding timing of delivery

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Cesarean section (C-section)

• Women with HIV RNA levels gt1,000 copies/ml
  C-section delivery
• Discuss risks associated with C-section delivery.
  Risks balanced with the potential benefits
  expected for the neonate
• Scheduled C-section delivery should be performed
  at 38 weeks gestation (rather than at 39)

52
Counseling regarding scheduled cesarean section
(C-section)

• Plasma HIV-1 RNA levels most recent value used
  when counseling a woman regarding mode of
  delivery
• HIV RNA levels lt1,000 copies/ml, No evidence to
  reduce transmission
• Unknown HIV RNA levels not on ARV or only on ZDV
  for prophylaxis, C-section reduces perinatal
  transmission

53
Budding virus from immune cell

• Tr. with undetectable viral load can occur
• ZDV ? VL at all levels
• ZDV should be given to all women in labor

54
MORBIDITY FROM CESAREAN SECTION

• International perinatal HIV group - no ?
• Marcollett 2002 -?morbidity cesarean 1.85
  elective Vs 4.17 emergency C/S
• Crubert 2002 ? postop. complications
  with ? immune status

55
Obstetric Intervention

• Avoid scalp electrode
• AROM
• Instrumental delivery
• Episiotomy
• Prolonged Induction
• External tocodynamometry

56
UNCLEAR ISSUES

• Role of PPROM and cesarean section
• Interval from PPROM to cesarean section
• Longer interval ? transmission short PPROM high
  load ? cesarean section

57
Other options

• Vaginal disinfection no ? in MTCT
• Vitamin A therapy
• Maternal baths
• Infant baths

58
Effect of Pregnancy on HIV

• No progression of disease
• Lowers CD4 count in all females

59
Obstetric outcome

• HAART therapy - no ? in PTD/IUGR
• No difference in outcome (US studies) (Minkoff
  90)
• Disparity noted in women from countries with
  inadequate treatment
• Anemia
• Low birth weight Chamiso 1996
• Leroy 1996

60
ACUTE FATTY LIVER
NORMAL
61
CLINICAL SCENARIOS
62
BEWARE OF POSTPARTUM

• Lactic acidosis
• Pancreatitis
• Mitochondrial fatty oxidation in fetus
• Follow LFT every 3-4 weeks last trimester
• Neonatal mitochondrial dysfunction
• ZDV Lamivudine

63
Breastfeeding and HIV Infection

• Breast feeding not recommended
• All Women considering breastfeeding should know
  their HIV status

64
Post-delivery recommendation

• Refer for specialty HIV care
• Possible changes in therapy
• Discontinue ZDV if given only to prevent
  perinatal transmission
• Start on combination ARV regimen or
• No ARV (if viral/immune parameters dont warrant
  therapy)

65
In Utero Exposure
66
Mitochondrial toxicity

• Affinity for mitochondrial DNA polymerase
• Depletion dysfunction
• Acute fatty liver
• Inability to oxidize fatty acids
• Genetic susceptibility to exposed infants

67
Antiretroviral Pregnancy Registry

• Collaborative project managed by PharmaResearch
  (OB/GYN, ID, teratology, epidemiology, CDC NIH)
  sponsored by
• Abbott Laboratories, Agouron Pharmaceuticals,
  Inc., Boehringer Ingelheim Company, Bristol-Myers
  Squibb, Co., Gilead Sciences, Inc.,
  GlaxoSmithKline, F. Hoffmann-LaRoche Ltd., Merck
  Co., Inc. and PharmaResearch.
• To assess safety of ARVs in pregnancy
• (800) 258-4263 Fax (800) 800-1052
  http//www.apregistry.com

68
Until all pregnant women have access to therapy,
the promise of ACTG 076 cannot be realized!
69
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70
Syphilis

• Treponema Pallidum
• Readily cross placenta
• Perinatal transmission
• Primary/secondary syphilis 50
• Early latent 40
• Late latent 10
• Tertiary 10

71
Clinical Phase Transmission
Primary Chancre 2-6 wks Infectious Secondary
Bacteremia gt 6 wk Infectious Latent Exacerbations
lt 1 yr from I Infectious Late Latent gt 1
yr Transplacental infn Tertiary CVS Not by
sex CNS Gummas MSK
72

• Primary Syphilis
• 3 6 wk of infections
• Secondary Syphilis
• Disseminated d z
• 6 wk 6 mo
• Latent syphilis
• Subclinical with or without relapse

73

• Congenital Syphilis
• 1.5/100,000 in Non-hispanics whites
• Declined by 21 from 2000- 2002
• Parallel with 35 decline of incidence of
  primary syphilis

74
Cong. Syphilis

• 80 occur due to inadequate meds
• Transplacental panape as early as 6 wks
• CF not seen until 16 wks
• Intrapartum, lesion from skin lesions

75
Perinatal Pathology

• Hydrops placentalis
• Villitis (plasmacell infiltrate)
• Villous proliferation around vessels (onion skin
  vessels)
• Funisitis
• Chrono ammionitis
• Plasma cell deciduitis

76
Fetus

• Depend on stage of development
• Abnormal liver function
• Hepatomegaly
• Low platelets
• Anemia
• Ascites

77
Infant Clinical Stigma
78
Maternal Screening

• Universal screening
• First visit
• III trimester delivery in high risk population
• Any still birth

79
Therapy

• Treat all women with positive titre unless
  adequate treatment history, clearly documented
  and decline in antibody titre documented

80
Treatment

• Primary, secondary early latent (lt1yr)
• Benzathine penicillin G, 2.4 m units IM x 1
• Late latent (gt1yr)
• 3 doses at 1 wk interval
• Penicillin allergic
• Confirm allergy desensitize

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Gonorrhea

• Incidence 0.5-7
• Transmission from infected male to female 50-90
• Incubation period 3 days
• Early bacteremic phase
• Septic arthritis phase, endocervicitis

83
Perinatal Complications

• Premature Rupture of Membrane
• Preterm Labor
• Chorioamnionitis
• Neonatal conjunctivitis (3-4 d)
• Corneal ulceration, scarring, blindness

84
Prevention

• Early diagnosis I visit
• Consider alternate site sampling
• Gram stain positive 60 only
• Amplified DNA probes (PACE 2 system)
• 20-50 co-existing chlamydia
• Reculture TOC (high risk)

85
Therapy

• 10 penicillin resistent
• Ceftriaxone 125 mg IM x 1
• OR
• Cifixime 400 mg PO x 1
• Azithromycin 1 gm PO x 1
• Amoxycillin 500 mg tid x 7 days
• Prophylactic agent into newborn life
• Erythromycin 0.5

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87
Cytomegalovirus

• CMV
• Double stranded DNA virus
• Horizontal transmission via
• Infected organ or blood
• Sexual contact
• Secretions Saliva, urine, vaginal
• Vertical transmission to fetus
• Transplacental infection
• Contaminated genital tract secretion
• Breast feeding

88
CMV

• 1-4 uninfected seroconvert
• Primary Inf, 40-50 fetus affected
• 5-20 of babies symptomatic at birth
• 30 severely infected fetus die
• 80 survive with morbidity
• Ocular abnormality
• Sensory neural hearing loss
• IUGR, ? LFT, ? Platelets
• Recurrent or reactivation less likely trans. But
  long term follow-up 15 hearing loss

89
Diagnosis

• IgM or increasing 1gG titres
• Amniotic fluid PCR or culture UBS
• Umbilical blood sampling
• USG, wnl - range of anomalies
• Microcephaly
• Intra cerebral calcification
• Hydrops, IUGR, Oligo
• Heart block, echogenic bowel, anemia
• Isolated serous effusions

90
Intrapartum

• Genital tract secretions (10 ? shed virus)
• 20-60 fetus shed virus from pharynx
• Postpartum breast feeding

91
Prevention

• No vaccine or meds in pregnancy
• Education Health care, daycare, school teachers,
  young mothers
• Risk of sexual transmission
• CMV free blood products
• Universal precautions
• Antivirals

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HSV

• HSV 1 above waist
• HSV 2 below waist
• True only 90 time
• Sero prevalence 25
• Pregnant women 0.02-1
• Asymptomatic preg. women 0.6

94
Clinical Findings

• I episode local symptoms 2-3 wks
• 2/3 acquired asymptomatically!!
• Recurrent lesion viral shedding 3-5 d

95
Perinatal Infection

• Transplacental rare reported cases
• Current genital HSV, higher incidence
• 50 infected fetus may not have lesions
• Infn acquired from infected genital tract
• Previous antibody lesion risk 1-2
• Infected infants 50-90 mortality morbidity

96
Diagnostic Pitfalls

• 1/3 of women no typical lesions
• Pap not reliable
• Viral culture false
• Others ELISA, PCR

97
Management

• All pregnant women, history, screen
• Serial cultures not recommended
• Specimen PCR

98
Therapy

• Supportive
• Therapeutic dose antiviral for primary infection
• Prophylatic chronic suppressive dose 3-4 wks
  prior to delivery
• Acyclovir
• Valacyclovir
• Famciclovir

99
Labor Management

• Precaution to present early
• If lesion CD, if not normal
• If lesion SROM, CD may not completely prevent
  transmission
• Non-genital herpes
• Gown glove precaution
• Linen dressing till lesion encrust

100
HPV

• More than 100 types of HPV
• 1 million new cases annually
• Smoking, prolonged OCP use ? risk
• Asymptomatic dz ? risk
• 40 sexually active women HPV
• 65 infection rate, ICP 3-8 m

101
Perinatal Transmission

• Transplacental rare
• Vaginal, cervical lesions
• Postpartum newborn (nb) contact
• 151 female 74/PCR (20,34,36 wk)
• Only 4 nb were positive (Watts, et al.)
• Follow up of 11 nb ve pts
• 30 nb ve at 5 wks
• All were ve at 18 mo (Tent, et al.)
• Suggest contamination vs infection
• Routine CD not recommended
• CD for obstructive lesions

102
Medication during Pregnancy

• Trichloroacetic acid
• Cryotherapy
• Surgical excision

103
Questions?

• Cincinnati HIV/STD Prevention Training Center
  Website
• http//www.stdptc.uc.edu
• Consultation Line 1-800-459-2820
• Email std.traincenter_at_cincinnati-oh.gov

104
Thank You!
105
Reminder Get your CMEs

• After viewing this eLearning Seminar, please go
  to our website, www.stdptc.uc.edu
• Sign in, look for the title of this seminar
• Follow directions to register
• Complete the evaluation
• Print out your CEU certificate!

106
Perinatal Transmission Of Infectious Disease
Oormila P. Kovilam, M.D. University of
Cincinnati Department of Obstetrics
Gynecology Cincinnati STD/HIV Prevention Training
Center