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Diagnosis of HIV Infection in Infants, Children and Adolescents
A. Test for HIV Antibody
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HIV Testing of Pregnant Women: HIV counseling and testing are recommended
as the standard of care for all pregnant women.
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HIV-testing should be offered as early as possible during the prenatal
period.
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If not tested during pregnancy, counseling and testing should be offered
to women during the postnatal period.
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HIV Testing of Neonates: HIV antibody testing, accompanied by appropriate
counseling of the mother, should also be the standard of care for neonates
born to mothers who have not received HIV antibody testing during pregnancy
or in whom antibody test results are not known to the pediatrician
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HIV Infection Status of Neonates: Infants at risk for HIV infection
(mother or infant is HIV-antibody positive) must have a determination of
their HIV infection status as soon as possible after birth.
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HIV Antibody by EIA: Highly sensitive (>99%) assays for HIV-1/HIV-2
antibodies. The presence of HIV antibody in an infant born to a mother
with HIV infection does not differentiate maternal from infant antibody.
Maternal antibody may be detected in the infant until 12-15 months.
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HIV-1-EIA: From 60-91% of HIV -2 infected persons will test repeatedly
reactive by HIV-1 EIA. A repeatedly reactive test must be tested by the
Western blot assay or by IFA to HIV-1 before reporting.
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HIV-2-EIA: HIV-2 infection is rare in the U.S. except in travelers
from West Africa or persons who have had sexual contact with West Africans
infected HIV-2. A repeatedly reactive test must be confirmed by a supplemental
test at the state laboratory.
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HIV-1/HIV-2 (rDNA) EIA (Abbott Lab): This test has been available
since February 1992 and test for both HIV types:
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Repeatedly reactive test: Must do HIV-1 WB or IFA assay.
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Repeatedly reactive test with negative or indeterminate WB: Must
do HIV-2 EIA, if repeatedly reactive do HIV-2 supplemental test
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Supplemental HIV test: Any repeatedly reactive HIV-1, HIV-2 or HIV-1/HIV-2
EIA test must be tested by one or more of these supplemental test before
reporting:
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HIV-1 Western Blot Assay: This assay test for antibodies to specific
HIV-1 proteins. This is a highly specific assay.
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Positive: A positive HIV-1 WB confirms the presence of antibodies
to HIV. Although this does not always distinguish between antibodies to
HIV-1 and HIV-2, further testing is not required for routine purposes.
If the suspicion of HIV-2 infection (based on epidemiologic risk factors
[ see appendix E]) is high, additional testing for HIV-2 is indicated.
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Negative: If the HIV-1 WB is negative, an EIA for HIV-2 only should
be performed. If the HIV-2 EIA is repeatedly not reactive, the specimen
should be considered negative for HIV antibodies.
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Indeterminate: If the HIV-1 WB is indeterminate, an EIA for HIV-2
only should be performed. If the HIV-2 EIA is repeatedly not reactive,
the specimen should be considered indeterminate. Repeat testing is advised
in 6 months to exclude the possibility of early HIV-1 infection.
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Immunofluorescent Assay (IFA) for HIV-1 Antibody:
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A positive or negative HIV-1 IFA should be interpreted in the same
manner as similar results from the WB test.
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An Indeterminate HIV-1 IFA should first be tested by HIV-1 WB and
reported based on its results as above.
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Supplement HIV-2 confirmatory test are not currently licensed, therefore
those specimens with repeatedly reactivity to HIV-2 EIA must be sent to
the state laboratory for further testing. The report will be positive,
negative or indeterminate with similar interpretation as for the supplemental
test for HIV-1.
B. Test for HIV Infection Status in Infants <18
months.
With the use of these tests:
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Approximately 50% of infected infants can be identified at or near birth.
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Greater than 95% of infected infants can be diagnosed by 3-6 months.
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At risk infants should have one or more of these tests performed as soon
as possible after birth and these test should be repeated between 3-6 months
of age.
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Seropositive infants who do not have a definitive virologic diagnosis of
HIV infection should continue to be tested every 3 months by ELISA/WB Assays.
After the first year, HIV antibody should be performed at 18 and 24 months
of age.
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Seroreverter: A child of an HIV-infected mother who is repeatedly
HIV-antibody-negative by 18 months of age and has never had a positive
HIV culture/PCR/P24 antigen is considered as a seroreverter.
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HIV Culture: Not readily available, large volume of blood required
and may require several weeks growth for detection.
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HIV-P24 Antigen Assay:
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Standard Assay: The P24 Antigen in the serum of infants is bound
to maternal HIV antibody. This test is insensitive for the detection of
HIV infection in infants. Less than 20% have detectable P24 antigen 1-6
months of age. It only detects free antigen.
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ICD-HIV-P24 Assay: If acid hydrolysis is used to disrupt antigen-antibody
complexes in serum, the sensitivity of P24 antigen detection can be increased,
and this assay may be a tool for early diagnosis. 100% are positive by
1-3 months of age.
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HIV-DNA-PCR: A highly sensitive and specific test for early detection
of HIV infection in infants. All infected infants detected by 6 months
of age.
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HIV-IgA Antibody Test: Maternal IgA antibodies do not cross the
placenta, therefore the detection of HIV specific antibodies in the infant
serum indicates the presence of HIV infection. This assay is insensitive
for the detection of infection in the first 3 months. (17% at one month,
67% at 3 months), but a very sensitive assay in infants 6 months. (94%
detected at 6 months, 100% detected 9 months). This assay is not yet commercially
available.
C. Immunologic Test:
To obtain in HIV-infected infants/children/adolescents
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Lymphocyte subsets: CD4, CD8 and CD4/CD8 ratio - Should be performed
on all infants born to HIV-infected mothers at 1, 3, and 6 months of age,
then every 3-months until HIV status of the child in known. - Should be
monitored every 3-6 months in children proven to be HIV-infected.
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Quantitative immunoglobulin: IgG, IgM, IgA
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Skin Test: Candida, Mumps, Tuberculin Skin Test (PPD)
D. Diagnosis of HIV infection in Children:
Optimally, all infants at risk for HIV infection should be diagnosed by
laboratory means well before clinical manifestations of HIV develop.
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Diagnosis: HIV Infected
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A child less than18 months of age who is known to be HIV seropositive or
born to an HIV-infected mother and:
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Has positive results on two separate determinations (excluding cord blood)
from one or more of the following HIV detection tests:
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HIV culture
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HIV - DNA-PCR
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HIV-P24 Antigen or
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Meets criteria for AIDS diagnosis based on the 1987 AIDS surveillance definition.
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A child 18 months of age born to an HIV-infected mother or any child infected
by blood, blood products, or other known modes of transmission (e.g. sexual
contact) who:
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Is HIV-antibody positive by repeatedly reactive EIA and confirmatory test
(e.g. WB or IFA) OR
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Meets any of the criteria in 1 above.
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Diagnosis: Perinatally Exposed
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A child who does not meet the criteria above who:
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Is HIV seronegative by EIA confirmatory test (e.g., WB or IFA) and is <18
months of age at the time of test; or
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Has unknown antibody status, but was born to a mother known to be infected
with HIV.
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Diagnosis: Seroreverter (SR)
A child who is born to an HIV-infected mother and who:
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Has been documented as HIV-antibody negative (i.e, two or more negative
EIA test performed at 6-18 months of age or one negative EIA test after
18 months of age); and
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Has had no other laboratory evidence of infection (has not had two positive
viral detection test, if performed); and
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Has not had an AIDS-defining condition.
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Criteria for HIV Infection for Persons >13 years:
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Repeat reactive screening test for HIV antibody (e.g. Enzyme Immunoassay)
with specific antibody identified by the use of supplemental test (e.g.
Western Blot, immunofluorescence assay)
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Direct identification of virus in host tissues by virus isolation.
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HIV antigen detection
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A positive result on any other highly specific licensed test for HIV
E. Classification of HIV Infection (CDC):
1. Pediatric HIV Classification
TABLE 1. Pediatric human immunodeficiency virus
(HIV) classification*
|
Clinical categories |
| Immunologic Categories |
N: No signs/symptoms |
A: Mild signs /symptoms |
B: **Moderate signs /symptoms |
C: **Severe signs/symptoms |
| 1: No evidence of suppression |
N1 |
A1 |
B1 |
C1 |
| 2: Evidence of moderate suppression |
N2 |
A2 |
B2 |
C2 |
| 3: Severe suppression |
N3 |
A3 |
B3 |
C3 |
* Children whose HIV infection status is not confirmed are classified
by using the above grid with a letter E (for perinatally exposed) placed
before the appropriate classification code (e.g., EN2)
** Both Category C and lymphoid interstitial pneumonitis in
Category B are reportable to state and local health departments as acquired
immunodeficiency syndrome.
TABLE 2. Immunologic categories based on age-specific CD4+
T-lymphocyte
counts and percent of total lymphocytes
| Immunologic Category |
| Age of Child |
| <12 mos |
1-5 yrs |
6-12 yrs |
| µL |
(%) |
µL |
(%) |
µL |
(%) |
| 1: No evidence of suppression |
>1,500 |
(>25) |
>1,000 |
(>25) |
>500 |
(>25) |
| 2: Evidence of moderate suppression |
750-1,499 |
(15-24) |
500-999 |
(15-24) |
200-499 |
(15-24) |
| 3: Severe suppression |
<750 |
(<15) |
<500 |
(<15) |
<200 |
(<15) |
Box 2. Clinical categories for children with human immunodeficiency virus
(HIV) infection
Category N: Not Symptomatic Children who have no signs or symptoms
considered to be the result of HIV infection or who have only one of the
conditions listed in Category A.
Category A: Mildly Symptomatic Children with two or more of the
conditions listed below but none of the conditions listed in Categories
B and C.
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Lymphadenopathy ( 0.5 cm at more than two sites; bilateral= one site)
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Hepatomegaly
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Splenomegaly
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Dermatitis
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Parotitis
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Recurrent or persistent upper respiratory infection, sinusitis, or otitis
media
Category B: Moderately Symptomatic
Children who have symptomatic conditions or other than those listed
for Category A or C that are attributed to HIV infection. Examples of conditions
in clinical Category B include but are not limited to:
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Anemia (<8 gm/dL), neutropenia (<1,000/mm3), or thrombocytopenia
(<100,000/mm3) persisting 30 days
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Bacterial meningitis, pneumonia, or sepsis (single episode)
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Candidiasis, oropharyngeal (thrush), persisting (>2 months) in children
>6 months of age
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Cardiomyopathy
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Cytomegalovirus infection, with onset before 1 month of age
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Diarrhea, recurrent or chronic
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Hepatitis
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Herpes simplex virus (HSV) stomatitis, recurrent (more than two episodes
within 1 year)
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HSV bronchitis, pneumonitis, or esophagitis with onset before 1 month of
age
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Herpes zoster (shingles) involving at least two distinct episodes or more
than one dermatome
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Leiomyosarcoma
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Lymphoid interstitial pneumonia (LIP) or pulmonary lymphoid hyperplasia
complex
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Nephropathy
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Nocardiosis
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Persistent fever (lasting >1 month)
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Toxoplasmosis, onset before 1 month of age
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Varicella, disseminated (complicated chickenpox)
Category C: Severely Symptomatic Children who have any condition
listed in the 1987 surveillance case definition for acquired immunodeficiency
syndrome (10), with the exception of LIP (Box 3)
Box 3. Conditions included in clinical Category C for children infected
with human immunodeficiency virus (HIV)
Category C: Severely Symptomatic*
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Serious bacterial infections, multiple or recurrent (i.e., any combination
of at least two culture-confirmed infections within a 2-year period), of
the following types: septicemia, pneumonia, meningitis, bone or joint infection,
or abscess of an internal organ or body cavity (excluding otitis media,
superficial skin or mucosal abscesses, and indwelling catheter-related
infections).
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Candidiasis, esophageal or pulmonary (bronchi, trachea, lungs)
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Coccidioidomycosis, disseminated (at site other than or in addition to
lungs or cervical or hilar lymph nodes)
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Cryptococcoses, extra pulmonary
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Cryptosporidiosis or isosporiasis with diarrhea persisting > 1 month
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Cytomegalovirus disease with onset of symptoms at age > 1 month (at site
other than liver, spleen, or lymph nodes)
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Encephalopathy (at least one of the following progressive findings present
for at least 2 months in the absence of a concurrent illness other than
HIV infection that could explain the findings): a) failure to attain or
loss of developmental milestones or loss of intellectual ability, verified
by standard developmental scale or neuropsychological tests; b)impaired
brain growth or acquired microcephaly demonstrated by head circumference
measurements or brain atrophy demonstrated by computerized tomography or
magnetic resonance imaging (serial imaging is required for children <2
years of age); c) acquired symmetric motor deficit manifested by two or
more of the following: paresis, pathologic reflexes, ataxia, or gait disturbance
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Herpes simplex virus infection causing a mucocutaneous ulcer that persists
for > 1 month; or bronchitis, pneumonitis, or esophagitis for any duration
affecting a child > 1 month of age
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Histoplasmosis, disseminated (at a site other than or in addition to lungs
or cervical or hilar lymph nodes)
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Kaposi's sarcoma
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Lymphoma, primary, in brain
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Lymphoma, small, noncleaved cell (Burkitt's), or immunoblastic or large
cell lymphoma of B-cell or unknown immunologic phenotype
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Mycobacterium tuberculosis, disseminated or extra pulmonary
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Mycobacterium, other species or unidentified species, disseminated (at
a site other than or in addition to lungs, skin, or cervical or hilar lymph
nodes)
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Mycobacterium avium complex or Mycobacterium kansasii, disseminated
(at a site other than or in addition to lungs, skin, or cervical or hilar
lymph nodes)
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Pneumocystis carinii pneumonia
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Progressive multifocal leukoencephalopathy
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Salmonella (nontyphoid) septicemia, recurrent
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Toxoplasmosis of the brain with onset at > 1 month of age
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Wasting syndrome in the absence of a concurrent illness other than HIV
infection that could explain the following findings:
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a) persistent weight loss >10% of baseline OR
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b) downward crossing of at least two of the following percentile lines
on the weight-for-age chart (e.g., 95th, 75th, 50th, 25th, 5th) in a child
1 year of age OR
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c) <5th percentile on weight-for-height chart on two consecutive measurements,
30 days apart
PLUS
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a) chronic diarrhea (i.e., at least two loose stools per day for 30 days)
OR
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b) documented fever (for 30 days, intermittent or constant)
* See the 1987 AIDS surveillance case definition (10) for diagnosis criteria.
Taken from A
Manual for the Management of HIV Infections in Infants, Children, and Adolescents
by William
S. Foshee, M.D., is an Associate Professor of Pediatrics at The Medical
College of Georgia/Children's Medical Center and Educational Coordinator
for Pediatrics at University Hospital in Augusta, Georgia.
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