6030 Exam 4 mod 12 HIV.pdf

Full Transcript

HIV and Primary Care
•

HIV
• Types of HIV
o HIV -1
§ More common worldwide
§ Easier perinatal transmission
• STOP breastfeeding
§ Reduced valiance with slower rate of CD4 and T-Cell decline
o HIV-2
§ Less easily transmitted
• Rare in the US à unless direct travel to West Africa
• HIV-2 may be dx when treatment is not working
§ Less pathogenic
• Period btw infection and symptoms is longer
§ Less likelihood perinatal transmission
• May need to stop breastfeeding

•

•

•

HIV vs AIDS
o HIV
§
§
§
o AIDS
§
§
§

Breaks down body’s defense
Infects specific white blood cells
Weakens immune system

Attacks the immune system
Reduces white blood cells
Symptoms or illnesses that result from HIV infection
• AIDS comes from HIV
HIV Transmission Categories
o Male to Male Sexual contact à Most Common
o Injection drug use
o Male to male sexual contact and injection drug use
o Heterosexual contact
o Perinatal
Goals of Care
o Diagnose à Establish Care à Retention in Care à Viral Suppression
§ Diagnose – 86%
• Screening in PCP
o Cultural humility
o Leave bias alone
o 14% Unaware of dx of HIV

Establish Care – 64%
• How soon can we start care
o (1mo or 30days is GOAL)
§ Retention in Care – 49%
• Follow up, engaged in the care à prevent further infection
§ Viral Suppression – 53%
• Get dx to start tx and get pt suppressed
Risk Factors for HIV
o Unprotected Intercourse
o Vaginal, Anal
o Needle sharing
o Perinatal Transmission – mother to baby
o Substance Abuse History - decrease adherence to safe practices
o Accidental Needle stick - occupational hazard
o Blood transfusion (prior to 1985)
o STIs
§ increase susceptibility for non-infected
§ increase of spread to others if already have HIV
o Mental Illness
§ Behavioral health support
Pathophysiology – 5 Stages
o Binding and entry
§ HIV varrions bind to glycoprotein to
help attach to CD4 receptors of a
susceptible cell à Interact with CD4
& CCR5 receptors to initiate fusion
btw the viral envelope and plasma
membrane to facilitate entry of the core of the virus to the cytoplasm
o Reverse transcription
§ RNA released
• RNA à DNA provirus à integrates into Host cell then into host
nucleus
o Integration
§ Into host DNA
o Synthesis of viral proteins
§ May be LATENT or ACTIVE
• Active: creates proteins
o Budding
§ Proteins bud then start cycle over
Natural Course of HIV
o Viral Transmission
o Acute Retroviral Syndrome
§ Primary Infection
§

•

•

•

• Presents like infectious mono
Increased Viral Load
• Period of Viral Replication
o > 1 Million Copies
o Recovery and Seroconversion
§ Antibodies develop (take up to 3mo)
• HIV Antibodies have NO protection
o Asymptomatic chronic HIV infection
§ Able to transmit (3mo-15yr)
• Shorter for children with HIV
o Symptomatic Infection
§ Physical Signs of HIV
o Death
Spectrum of Infections: Acute HIV Infection S/S
o Common:
§ Fever
§ Adenopathy
Cough is NOT part of
§ Sore Throat
Acute HIV infections
§ Rash
§ Myalgia
§ HA
§ Night Sweats
o Occasional (<50%)
§ Oral Ulcers
§ Thrombocytopenia
§ Leukopenia
§ Diarrhea
§ Nausea
§ Elevated ALT or AST
§ Aseptic Meningitis
Initial History
o HIV test
§ When? Why? Previous test, if any? Results?
o Thorough sexual hx
o PMH
o MH childhood trauma
o Family Hx
o Social Hx
o Housing and support
Exam
o Skin à Kaposis Sarcoma
§ Purplish Lesions à sign of AIDS
o HEENT
§

•

•

•

•

•

•

§ Eye Exam, Sinus tender, fund exam
§ Thrush à indicates disease progression
o Lymph Nodes
o Chest
§ Murmur, PCPneumonia à normal lung sounds
• CXR
o Abdomen
§ Enlarg liver and spleen
o Rectum/Genitalia
§ Cervical Carcinoma
o Neuro
§ Detailed exam à myopathy, neuro changes
Initial Labs
o CBC with differentials à anemias
o CMP à get baselines
o Urinalysis à Proteinuria
o Hepatitis serologies à best
o RPR à Syphlis co-infection
o Gonorrhea/Chlamydia à STI check
o Cytomeglavirus/ Toxoplasmosis
o HLA B* 5701 à test for hypersesnitivy and SJS risk
o Other labs to consider:
§ Fasting Blood Sugar
§ Lipid panel à ART increase Lipids
§ Hemoglobin A1c
§ Pap Smear with GC/CT
§ Oral swab (GC/CT)
§ Anal swab
Additional Labs (typically done by infectious disease)
o HIV Viral Load (or HIV RNA)
§ Idea of severity, cannot determine duration
o CD4 T-cell count/percentage (200/14)
§ Idea of immune system
§ More info about % of WBC
§ Best test for progression and for dertemining ART
o Resistance testing – Genotype and Phenotype
§ Baseline resistane info for tx
o Quantiferon or T-spot (substitution for PPD)
§ TB test
o Toxoplasmosis and Cytomeglovirus (CMV) IgG
o Glucose 6 Phosphate Dehydrogenase (G6PD)
o Dilated retina exam (especially if CD4 count <50)
o Tropism Assay
Plan of Care

Patient’s desires
How long since diagnosis
Motivation to succeed over time
Barriers and facilitators to
§ Care
§ Medication adherence
o Access to care, support services, medications
o History with medical care
o Patient’s social, emotional, spiritual milieu
o
o
o
o

•

ART: Antiretroviral Therapy
o Five Major Classes
§ 1. Nucleoside Reverse Transcriptase Inhibitors (NUKES)
• Works on Reverse Transcription
§ 2. Non-nucleoside Reverse
Transcriptase Inhibitors
• Works on Reverse
Transcription
§ 3. Protease Inhibitors
• Hinders develop of protein
§ 4. Fusion inhibitors/Entry Inhibitors
• Injury prevent stop the CCR5 receptors of cell and enter host cell
§ 5. Integrase Inhibitors
• Prevent from RNA integrate into host DNA
• When to start ART
o “ART is recommended for all HIV-infected individuals.”
§ Pregnancy
• Prevent transmission to fetis
§ History of AIDS-defining illness
• Thrush, KS (rash lesion)
§ HIV-associated nephropathy (HIVAN)
• Attack renal à seen in labs
§ Hepatitis B (HBV) coinfection
• Some ART treat both
§ Age > 50 years
• Because delayed immunity
• Typical Treatment
o Two NRTIs + 3rd Drug
§ 2 NUKES and another

•

Balance Now Favors Early ART

•

Potential Benefits of Early Therapy
o Potential decrease in risk of many complications, including:
§ HIV-associated nephropathy (HIVAN)
§ Liver disease progression from Hepatitis B or C
§ Cardiovascular disease
§ Malignancies (AIDS defining and non-AIDS defining)
§ Neurocognitive decline
§ Blunted immunological response owing to ART initiation at older
age
§ Persistent T-cell activation and inflammation
Consider Deferral of ART
o Clinical or personal factors may support deferral of ART
§ If CD4 count is low, deferral should be considered only in unusual
situations, and with close follow-up
• Low CD4 = Need meds
o When there are significant barriers to adherence
o If co-morbidities complicate or prohibit ART
Unique Side Effects with ART
o Peripheral neuropathies and pancreatitis
o Hypersensitivity with Abacavir à test HALB5701 for SJS
o CNS toxicity (EFV)
§ dizziness, aggravation of mental health complications, vivid dreams
• DO not give to those who suffer from PTSD or military

•

•

•

•

•

•

o Metabolic complications
§ Lipid abnormalities, altered glucose metabolism, body fat
redistribution, mitochondrial toxicity, neuropathies.
Immune Reconstitution Inflammation Syndromes (IRIS)
o IRIS: 3 types
§ Undx comorbidities can be heightened with ART therapy
o Practical definition
§ Paradoxical worsening of a preexisting infection of a previously
undiagnosed condition
o Paradoxical IRIS
§ Improvement of known infection with treatment but deteriorate
with ART
o Unmasking IRIS
§ Detection of previously unknown pathogen that shows a
prominent clinical expression with immune recovery
Prophylaxis Regimens
o Prevention of Opportunistic Infection – CD4 determines not symptoms
§ T-cell Count Driven
§ Pneumocystis Jiroveci pneumonia, CD4 <200
• No allergy to Sulfa à Bactrim DS 1 tab QD or QOD
• Allergy to Sulfa and G6PD sufficient: Dapsone 100mg QD or
Aerosolized Pentamidine Inhalation monthly
• G6PD insufficiency: Mepron 750mg BID
§ Mycobacterium Avium Complex, CDV <50
• Zirthromax IG weekly or Clarithromycin 500mg BID
§ Toxoplasmosis IgG positive and no active disease (CD4)
• Bactrim DS 1 tab daily
•
Follow Up
o Labs
o 1 month after initiating therapy
§ CBC with diff; CMP; CD4+, CD4%, HIV viral load
§ 3– 6 months: CBC with diff; CMP; CD4+, CD4%, HIV viral load
• Lipid panel and Hemoglobin A1c every 6 months
§ Goal: <40 copies or “undetectable”
o With each visit check mouth, lymph nodes, feelings, and emotions, and
well being
Prevention: Behavior Modification
o Consistent condom use
o Monogamy vs Partner reduction
o Safer sex and drug practices

o Opiate substitution treatment à Methadone
o Prevention message every clinic visit
o Screen and treat for mental health
•

HIV Primary Care Considerations
o Consider
§ Vaccines/Immunizations
§ Preventative Screenings
§ Co-Morbidities
§ DDI
o Vaccines/Immunizations
§ Follow CDC Schedule for Immunocompromised
• HEP B àget titler 1 mo post vaccine
o Low CD4 wait for vaccine
• Pneumonia
o 13
o 23 à get >200 CD4
• HPV: 3 series
o 13-26 year olds
• Tdap = every 10 years
• Influenza annually
• Herpes Zoster
o 60+ and >200 CD4
• Meningococcal: 2 series
o College student
§ Having a HIV not a reason
o ROUTINE SCREENINGS

•

PREVENTATIVE SCREENINGS

•

•

•

Metabolic Co-Morbidities
o Dyslipidemia
o Diabetes Mellitus
o HTN
§ Others
o ***Chronic infection and inflammation increase risk of co morbidities
Metabolic Comorbidities and HIV
o Clinical Implications
§ Physical Change à Weight Gain
§ Hypertriglyceridemia
§ Low HDL
§ Increase LDL
§ Increased diastolic BP
§ Increased Metabolic syndrome profile
§ Increased cardiovascular risk

Dyslipidemia
o Treatment
§ High Intensity Statin
• Lowers LDL by >50%
§ Moderate Intensity Statin
• Lowers LDL by 30-50%
§ Low Intensity Statin
• Lowers LDL by <30%
o Choices:
§ Rosuvasatin

§ Atrovastatin
§ Pravastatin
o Contraindicated (with PIs)
§ Lovastatin
§ Simvastatin
o Other
§ Fibric Acids
§ Bile Acid Sequestrants (BAS)
§ Nicotinic Acid
•

What to look for
o Target measurements
o BMI
o Hypothyroidism
o Metabolic Syndrome
o Primary vs Secondary
o ASCVD risk
o Hepatotoxicity
o Hypertriglyceridemia
§ Pancreatitis
o Myopathy
o Diabetes/Insulin Resistance
o Neuro Concerns

•

Diabetes Mellitus
o Impaired glucose tolerance
o Insulin resistance
o Dyslipidemia
o Lipodystrophy
o Mitochondrial dysfunction
o
What to look for
o Target Measures
o BMI
o Metabolic
Syndrome
o Type 1 vs Type 2
o ASCVD risk
o Lipodystrophy
o Dyslipidemia
o Lactic acidosis
o Nephrotoxicity
o Complications
related to DM

•

•

Hypertensions
o Chronic inflammation by HIV causes enlarge and stiffening
o What to Look for:
§ Goal BP: 140/90
§ BMI
§ Metabolic Syndrome
§ ASCVD risk
§ Renal Insufficency
§ Dyslipidemia
§ DM
§ Proteinuria
§ Complications related to
HTN

o Non Pharm Approach
§ Diet
§ Exercise
§ Alcohol
§ Weight
§ Tobacco Cessation
•

Common Problems in HIV Care
o Folliculitis
o Candida
§ Oral, Esophageal, Rectal, Vaginal
o Herpes Simplex
o Herpes Zoster
o Anal Fistula
o Genital Warts (HPV)
o P. jirovecii (PCP)
o Toxoplasmosis

o Mycobacterium avium complex (MAC)
o Histoplasma capsulatum
o Coccidioidomycosis
•

Drug-Drug Interactions
o Vitamins
o Tums
o Oral Contraceptives
o PPIs
o ABX
§ Increased risk of C.Diff
o Steriods
o Fluticasone and Advair
§ Increase steroid toxicity
§ Immuno deficiency

•

Special Considerations
o Pregnancy - Contraception and preconception care
o Children - Advisory Committee on Immunization Practices for HIV-infected infants
and children
o Adolescents -Transition to adult care
o Transgender Care - Address specific biological, psychological, and social needs

•

Occupational Risk Exposures in Health Care Personnel
o Types of Stick:
§ Percutaneous Injury (needlestick,cut)
OR
§ Contact of mucous membrane or non-intact skin
o WITH:
§ Blood
§ Tissue
§ Other body fluids that are potentially infectious (cerebrospinal, synovial,
pleural, pericardial, peritoneal, or amniotic fluids: semen or vaginal
secretions)
o NOT Considered Infectious for HIV, Unless visibly bloody
§ Feces
§ Nasal Secretions
§ Salvia
§ Sputum
§ Sweat
§ Tears
§ Urine
§ Vomit

•

PEP: Initiating Post-Exposure Prophylaxis
o PEP should be started as soon as possible, preferably within 72 hours of an
exposure.
o 28 day course recommended for persons exposed to someone with a known HIV
status or someone whose status is unknown
o Three drug regimen recommended
§ Maximal suppression of viral replication
§ Resistance protection

o PEP Evaluation
§ Regardless if provider is taking PEP, reevaluation must occur within 72
hours, especially as additional information about the exposure or source
patient becomes available
§ If the source is found to be negative, PEP should be discontinued
§ Rapid HIV testing of the source patient can facilitate decisions regarding
PEP when the source patient’s HIV status is unknown
o Monitoring
§ Baseline
• HIV antibody test
• Hep B and C
• CBC, CMP
• HCG
§ After initiating ART
• HIV antibody test
o If symptomatic
o 6 weeks
o 12 weeks
o 6 months
• Hepatitis C
o 12 weeks
o 24 weeks
• Drug toxicities
o HIV antibody test, CBC, CMP, and HIV RNA
• Side effects
o Toxicity of Post Exposure Prophylaxis (PEP) Regimens
§ PEP should be given for a full 4 weeks
§ Side effects of ART drugs are common, and a major reason for not
completing PEP regimens

§

•

Therefore, to the extent possible, regimens that are tolerable for
shortterm use should be selected

PREP – Pre-Exposure Prophylaxis
o TDF/FTC or Truvada®
§ All persons at risk through sex or injection drug use.
o TAF/FTC or Descovy®
§ All persons at risk through sex, excluding those at risk through vaginal sex.
o Who should receive PrEP?
§ Sexually active gay and bisexual men without HIV
§ Sexually active heterosexual men and women without HIV
§ Sexually active transgender persons without HIV
§ Persons without HIV who inject drugs
§ Persons who have been prescribed nonoccupational post-exposure
prophylaxis (PEP) and report continued risk behavior, or who have used
multiple courses of PEP
o Monitoring
§ At least every 3 months
• Repeat HIV testing and assess for signs or symptoms of acute
infection
• Repeat pregnancy testing for women who may become pregnant
• Assess side effects, adherence, and HIV acquisition risk behaviors
• Monitor adherence and sexual behaviors
§ At least every 6 months
• Monitor creatinine clearance.
• Conduct STI testing recommended for sexually active adolescents
and adults
§ At least every 12 months
• Evaluate the need to continue PrEP as a component of HIV
prevention