Title: HIV INFECTION AND THE ACQUIRED IMMUNODEFICIENCY SYNDROME (AIDS)
1HIV INFECTIONAND THE ACQUIRED IMMUNODEFICIENCY
SYNDROME (AIDS)
2HISTORICAL PERSPECTIVES OF AIDS
- Recognition of Pneumocystis carinii pneumonia
(PCP) and Kaposis sarcoma (KS) in young healthy
men in NYC and Los Angeles - GRID to AIDS by CDC
- Isolation of Lymphadenopathy-Associated Virus
(LAV) by Pasteur Institute (Luc Montagnier) - Isolation of Human T-Lymphotrophic Virus , Type
III (HTLV-III) by NCI/NIH (Robert Gallo) - Recommendation of the name Human Immunodeficiency
Virus (HIV) by an international subcommittee on
virus taxonomy
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7HUMAN IMMUNODEFICIENCY VIRUSES (HIV)
- Classification
- Retroviridae (family)
- Lentivirus (genus)
- Characteristics
- 100 nm in diameter
- Genome of 2 single strands of RNA
- Nine genes
- Reverse transcriptase
- RNA-dependent DNA polymerase
- Transcribes RNA into DNA
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11GENOME OF HIV
- Contains 6 regulatory genes
- Contains 3 structural genes
- Env (Envelope glycoproteins)
- gp120 and gp41
- Gag (Core and matrix proteins)
- p55, p40 and p24
- Pol (Enzymes)
- Reverse transcriptase (p66, p51)
- Protease (p11)
- Integrase (p32)
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13HUMAN RETROVIRIDAE (EXOGENOUS RETROVIRUSES)
- Seven genera
- Alpha, Beta, Gamma, Delta, Epsilon, Lenti and
Spuma - Deltavirus
- Human T-lymphotropic virus, type I (HTLV-1)
- Human T-lymphotropic virus, type II (HTLV-II)
- Lentivirus
- Human immunodeficiency virus, type 1 (HIV-1)
- Human immunodeficiency virus, type 2 (HIV-2)
14CLASSIFICATION OF THE HUMAN IMMUNODEFICIENCY
VIRUSES (HIV)
- Types
- Human immunodeficiency virus, type 1 (HIV-1)
- Human immunodeficiency virus, type 2 (HIV-2)
- HIV-1 is divided into groups
- M (Major)
- N (New)
- O (Outlier)
- Group M is divided into
- Subtypes (Clades)
- Circulating recombinant forms (CRF)
15CLASSIFICATION OF HIV
16ORIGIN OF HUMAN IMMUNODEFICIENCY VIRUSES
- Existed as monkey virus in equatorial Africa
- HIV-1
- Chimpanzee (Pan troglodytes troglodytes)
- HIV-2
- Sooty Mangabey (Cercocebus atys)
- Transition from monkeys to humans
- When - Circa 1908
- Molecular phylogenetics
- How Hunter theory
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19MECHANISM OF PATHOGENICITY OF HIV
- Envelope protein (gp120) of HIV binds with CD-4
receptor on surface of - T-lymphocytes
- Macrophages
- Dendritic cells
- Microglial cells
- Coreceptors for attachment of HIV
- CCR5 (T-cells, macrophages, dendritic cells,
microglial - cells)
- CXCR4 (T-cells)
20MECHANISM OF PATHOGENICITY OF HIV
- Early infection
- CCR5 coreceptor is used (R5 strains)
- Growth equal in monocytes and lymphocytes
- Non syncytium-inducing (NSI)
- Late infection
- CXCR4 coreceptor is used (X4 strains)
- Growth in T cells
- Syncytium-inducing (SI)
- Emergence of X4 strains associated with
accelerated decline in CD4 T cells - Cause or consequence?
21MECHANISM OF PATHOGENICITY OF HIV
- Following attachment, virus enters cells and
removes protein coat - Viral RNA is transcribed into DNA by
- Reverse transcriptase
- Viral DNA then integrated into host cell DNA
- Integrase
- Integrated viral DNA
- Referred to as provirus
- Production of active infection
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24EPIDEMIOLOGY OF HIV INFECTION AND AIDS
- Since 1981, 65 million people worldwide have
contracted HIV - gt 25 million deaths
- 87 of HIV cases in developing nations
- 64 in sub-Saharan Africa
- 23 in southern and Southeast Asia
- Since 1981, 1.5 million people in the U.S. have
contracted HIV - Approximately 576,000 deaths
- In 2009, 56K new cases in the U.S.
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27TRANSMISSION OF HIV INFECTION AND AIDS
- Sexual intercourse with infected person
- Homosexual (MSM)
- Heterosexual
- Bisexual
- Children born to infected mothers
- Perinatal
- IV drug addicts sharing contaminated
syringes/needles - Transfusion of blood and blood products
- Transfusion recipients
- Hemophiliacs
- Occupational exposure in health-care setting
28CDC CLASSIFICATION OF HIV INFECTION AND DISEASE
IN ADULTS AND ADOLESCENTS
- Latest revision in 1993
- Clinical Categories
- A
- B
- C
- CD4 T Cell Categories (Absolute number or )
- gt 500/uL or gt 29 of total lymphocytes
- 200 499/uL or 14-28 of total lymphocytes
- lt 200/uL or lt 14 of total lymphocytes
29CDC CLASSIFICATION SYSTEM
CD4 Cell Categories Clinical Categories Clinical Categories Clinical Categories
CD4 Cell Categories A Asymptomatic, Acute HIV, or PGL B Symptomatic Conditions, not A or C C AIDS-Indicator Conditions
(1) gt 500 cells/µL A1 B1 C1
(2) 200-499 cells/µL A2 B2 C2
(3) lt 200 cells/µL A3 B3 C3
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32CDC CLASSIFICATION SYSTEM(CLINICAL CATEGORY A)
- Following initial infection
- Asymptomatic
- Acute Retroviral Syndrome
- Infectious mononucleosis-like or flu-like illness
- 2 days to 4 weeks following infection
- Clinical manifestations
- Fever, headache, lethargy, pharyngitis, myalgias,
photophobia, lymphadenopathy and a faint
maculopapular rash - Resolution within 30 days
- Persistent generalized lymphadenopathy (PGL)
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35CDC CLASSIFICATION SYSTEM (CLINICAL CATEGORY B)
- Symptomatic conditions not meeting conditions of
clinical categories A or C - Herpes zoster (shingles)
- Oropharyngeal Candidiasis (thrush)
- Candida albicans
- Vulvovaginal candidiasis
- Bacillary angiomatosis
- Bartonella henselae
- Peripheral neuropathy
- Idiopathic thrombocytopenic purpura (ITP)
- Hairy leukoplakia (oral)
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40CDC CLASSIFICATION SYSTEM (CLINICAL CATEGORY C)
- Acquired Immunodeficiency Syndrome (AIDS)
Defining Conditions - Esophageal Candidiasis
- Cryptosporidiosis
- Pneumocystis jiroveci (carinii) pneumonia
- Tuberculosis (pulmonary or extrapulmonary)
- Disseminated Mycobacterium avium complex (MAC)
disease - Histoplasmosis (disseminated or extrapulmonary)
41HIV INFECTION IN ADULTS (CLINICAL CATEGORY C)
- Acquired Immunodeficiency Syndrome (AIDS)
Defining Conditions - HIV wasting syndrome
- Cryptococcal meningitis
- Cytomegalovirus retinitis
- Cerebral Toxoplasmosis
- Progressive multifocal leukoencephalopathy (PML)
- JC virus
- Kaposis sarcoma
- Human herpesvirus type 8 (HHV-8)
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52PROGNOSIS AND MONITORING OF HIV TREATMENT AND
DISEASE
- CD4 T cell count (Immunological response)
- Absolute number
- Best indicator for patients with counts lt 200
cells/uL - Percent
- Best indicator for patients with counts gt 200
cells/uL - HIV-1 RNA (Viral load) (Virological response)
- Discordant immunological and virological
responses exist
53TREATMENT OF HIV INFECTION AND DISEASE
- Anti-retroviral drugs do not cure HIV infection
or disease - Suppression of virus to undetectable levels
- Suppression of virus
- Drugs must be taken continuously
- Patients remain infectious
- Mutation rate in HIV is high and resistance
develops - Recommendation for combination therapy
- Combination of drugs from two or more classes
- Highly Active Anti-Retroviral Therapy (HAART)
54TREATMENT OF HIV INECTION AND DISEASE
- Classes of anti-retroviral drugs
- Reverse Transcriptase Inhibitors (RTIs)
- Nucleoside
- Nucleotide
- Non-nucleoside
- Protease Inhibitors (PIs)
- Fusion or Entry Inhibitors
- Act on gp41 or CCR5 coreceptor
- Integrase Inhibitors
- Fixed dose combinations
- Drugs from two or more classes into a single
product
55TREATMENT OF HIV INECTION AND DISEASE
- Reverse transcriptase inhibitors
- Nucleoside analog (NARTI, NRTI)
- Converted into nucleotide
- Incorporated into and stops viral DNA synthesis
- Zidovudine (Retrovir)
- Nucleotide analog (NtARTI, NtRTI)
- Incorporated into and stops viral DNA synthesis
- Tenofir (Viread)
- Non-nucleoside (NNRTI)
- Not incorporated into viral DNA
- Binds to enzyme and inhibits function
- Nevirapine (Viramune)
56TREATMENT OF HIV INECTION AND DISEASE
- Goals of HAART
- Suppression of HIV
- Decrease viral load
- Reduce potential for resistance to anti-viral
agents - Immune system reconstitution
- Restore CD4 T cell population
- Immune system reconstitution
- Most successful with high baseline CD4 count at
HAART initiation - Increase of 50 to 150 cells per year
57TREATMENT OF HIV INECTION AND DISEASE
- HAART negatives
- High cost, medication fatigue, adherence to
complicated drug regimens, adverse events, names
for anti-retroviral drugs - HAART Interruption
- Minimize negatives using structured treatment
interruption (STI) - 6 months of IL-2 without HAART
- Safety (unclear) and efficacy (inferior)
- HAART associated with
- Immune reconstitution syndrome
58IMMUNE RECONSTITUTION SYNDROME (IRS)
- Immune reconstitution inflammatory syndrome
(IRIS) - Strong response by recovering immune system to
latent or active infections - Risk factors for IRIS following HAART
- CD4 percent of lt 15
- CD4 count of lt 100 cell/uL
- High rate of increase of CD 4 count
- Most commonly associated with
- Pneumocystis pneumonia
- Cytomegalovirus disease
- Herpes zoster
- Mycobacterium avium complex (MAC) disease
- Tuberculosis
59IMMUNE RECONSTITUTION SYNDROME
- Important to distinguish between IRIS and
clinical failure - Clinical failure
- Disease progression with development of OI or
malignancy when drugs given for sufficient time - IRIS
- Seen within first several weeks of therapy when a
latent or active infection is present
60IMMUNE RECONSTITUTION SYNDROME
- Management options
- Inflammatory reaction treated with
- Steroids
- Non-steroidal anti-inflammatory drugs (NSAIDS)
- Antimicrobial agents directed at the infectious
agent - Antiretroviral therapy
- Withhold or continue (?)
61NAMING ANTI-RETROVIRAL DRUGS
- Anti-retroviral drugs have at least 3 names
- Abbreviation
- Research or chemical name
- Generic name
- Generic name
- Trade name
- Example
- Abbreviation (Research/Chemical) AZT
- Abbreviation (Generic name) ZDV
- Generic
Zidovudine - Trade
Retrovir
62MARAVORIC (MVC / SELZENTRY)
- First in new class anti-retroviral drug
- CCR5 co-receptor antagonist (entry inhibitor)
- Indicated for CCR5 tropic HIV-1 showing
resistance to multiple anti-retroviral drugs - Black box warning
- Hepatotoxicity
- Systemic allergic reaction
- Pruritic rash, eosinophilia, elevated IgE
- FDA approval on August 8, 2007
- Requires tropism testing
63HIV CO-RECEPTOR TROPISM ASSAY
- Trofile (Monogram Bioscience)
- FDA approval on August 6, 2007
- In vitro diagnostic assay
- Determines tropism of patients HIV
- CCR5
- CXCR4
- D/M (dual / mixed)
- Trofile assay
- Specimen is EDTA plasma
- Viral load of 1,000 copies/mL
- TAT of 14 days
- Cost
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66LABORATORY DIAGNOSIS OF HIV INFECTION
- Standard algorithm consists of using two tests
for the detection of antibody to HIV-1/2 - Screening
- Enzyme immunoassay (EIA) or
- Enzyme-linked Immunosorbent Assay (ELISA)
- High sensitivity
- Confirmation
- Western blot (WB)
- High specificity
- Sensitivity is positivity in disease
- Specificity is negativity in disease
67LABORATORY DIAGNOSIS OF HIV INFECTION (STANDARD
ALGORITHM)
- Specimens initially reactive by EIA / ELISA are
retested in duplicate - One or both repeat tests positive, specimens are
considered repeatedly reactive for antibody - Specimens repeatedly reactive by EIA / ELISA
then tested by Western Blot (WB) assay - Specimens reactive for both EIA / ELISA and WB
are considered positive for HIV infection - Seroconversion
- From infection to antibody
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69LABORATORY DIAGNOSIS OF HIV INFECTION
- Rapid detection of HIV-1/2 antibody
- OraQuick ADVANCE Rapid HIV-1/2 Antibody
- OraSure Technologies, Inc., PA
- Immunochromatographic assay (ICA)
- Analytical time of 25 minutes
- Sensitivity of 99.5 and specificity of 99.9
- Specimens of Choice
- Whole blood
- Fingerstick
- Venipuncture (EDTA)
- EDTA plasma
- Oral fluid (Oral mucosal transudate)
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72CLINICAL USE OF ORAQUICK RAPID HIV-1/2 ASSAY
- Rapid screening
- HCW with potential HIV exposure
- Pregnant females with unknown HIV status at time
of delivery - New HIV clinic patients
- Same day screening
- All other patients
- Reporting of Results
- Negative for HIV-1/2 Antibodies
- Preliminary Positive for HIV-1/2 Antibodies.
Confirmation by Western Blot testing to follow.
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78LABORATORY DIAGNOSIS OF HIV INFECTION
- Detection of HIV Core Antigen (p24)
- Serum or CSF
- Methods
- EIA or ELISA (Non-ICD)
- EIA or ELISA (immune complex dissociation)
- Positives confirmed by neutralization
- Clinical Use
- Early diagnosis before antibody response
- Monitor effectiveness of therapy
- Marker of disease progression
79LABORATORY DIAGNOSIS OF HIV INFECTION
- Detection of proviral DNA
- EDTA whole blood
- Method
- Polymerase chain reaction (PCR)
- Clinical Use
- Diagnosis of infection in neonates of HIV
positive mothers - Early diagnosis before antibody response
80LABORATORY PROGNOSIS OF HIV INFECTION
- Quantitation of HIV-1 RNA (Viral load)
- EDTA plasma
- Methods
- Reverse Transcriptase PCR (RT-PCR)
- Branched chain DNA (bDNA)
- Clinical Use
- Determination of amount of free virus (Viral
load) - Predicting progression and outcome of infection
- Assessing efficacy of antiviral therapy
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82LABORATORY DIAGNOSIS OF HIV INFECTION BY ORAL
FLUID TESTING
- OraQuick ADVANCE Rapid HIV-1/2 Antibody Test
- Pad on test device used to swab between upper and
lower outer gums and cheek - Pad is stored in preservative vial and sent for
ICA testing - Advantages
- Reduces occupational exposure
- Patient appeal
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84LABORATORY DIAGNOSIS OF HIV INFECTION BY URINE
TESTING
- Calypte HIV-1 Urine EIA (Calypte Biomedical,
Berkeley, CA) - FDA approval for EIA (1996) and Western Blot
(1998) - Sensitivity and specificity
- Lower compared to blood and oral fluid
- Question
- IgG in urine
- Calypte Aware HIV-1/2 Urine Rapid Test
- Available outside US
- Advantages
- Reduces occupational exposure
- Patient appeal
85THE IMMUNOLOGY OF HIV INFECTION
- Interactions between HIV and human immune system
are extremely complex - HIV subverts immune system by
- Infecting CD4 T cells and inducing quantitative
and qualitative dysfunction - Hyperactivating B cells with resulting
hypergammaglobulinemia - Inducing cytokine system to own replicative
advantage - There are no known correlates of protective
immunity
86MECHANISMS OF CD4 T-CELL DEPLETION
- Direct killing of infected T cells
- Increased rate of apoptosis in infected T cells
- Molecule associated with apoptosis (PD-1) is
over-expressed in chronic viremia - Syncytia formation
- Fusion of infected and non-infected T cells
- Killing of infected CD4 cells by CD8 cells
87KILLING OF INFECTED CD4 CELLS BY CD8 CELLS
ALTERNATIVE VIEW
- Mechanism that keeps HIV in check in long term
non-progressors (LTNPs) - Long term non-progressors (LTNPs)
- Carry the virus but do not get AIDS
- Have 20 times more CD8 T cells than progressors
- Function of CD8 T cell surplus
- Up-regulate production (2X rate of progressors)
of 2 killer proteins - Perforin
- Granzyme B
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89IMMUNE DYSFUNCTION DURING HIV INFECTION - SUMMARY
- HIV infection is multifactorial process capable
of disarming immune system by direct and indirect
mechanisms - Certain chemokine receptors function as necessary
coreceptors for entry of HIV into cells - Central Paradox
- Progression of HIV disease in setting of vigorous
immune response - Lack of correlates of protective immunity are
major obstacle to immunotherapy and vaccine
development
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