Human immunodeficiency virus: Difference between revisions
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==Background== |
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* A chronic immunodeficiency resulting from infection with the human immunodeficiency virus (HIV) |
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* Acquired immune deficiency syndrome (AIDS) is a severe form of HIV characterized by low CD4 count resulting in characteristic infections |
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*A chronic immunodeficiency resulting from infection with the human immunodeficiency virus (HIV) |
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== Microbiology == |
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*Acquired immune deficiency syndrome (AIDS) is a severe form of HIV characterized by low CD4 count resulting in characteristic infections |
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===Microbiology=== |
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* A member of the Retroviridae family |
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*A member of the Retroviridae family |
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=== Clades / Subtypes === |
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*Clades or subtypes: |
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**HIV-1: by far the most common species worldwide |
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***M group |
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****Clade A: common in East Africa |
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****Clade B: is common in Canada, Americas, Europe |
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**HIV-2: essentially confined to West Africa and certain parts of southern Europe and Asia |
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===Life Cycle=== |
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* HIV-1 |
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** M group |
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*** Clade A: common in East Africa |
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*** Clade B: is common in Canada, Americas, Europe |
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* HIV-2 |
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*Two phases: initial viral attachment, fusion, reverse transcription, and integration; and the following lifetime of the viral infection |
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== Life Cycle == |
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*Initial cellular infection |
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*#Binding or attachment of the virion gp120 Env surface protein to the CD4 receptor with CCR5 or CXCR4 coreceptor (on macrophage or T-cell, respectively). |
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*#Binding the receptor triggers a conformational change that exposes the fusion domain on gp41, which facilitates fusion and viral entry. The proceeding viral disassembly requires viral protein p24 to bind to cellular cyclophilin A. |
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*#In the cytoplasm, reverse transcriptase converts viral RNA into viral DNA. The RNA is degraded, then the complementary strand of DNA created. |
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*#The preintegration complex of double-stranded DNA is imported into the nucleus using viral Gag, viral protein R (Vpr), and integrase. Unlike other retroviruses, HIV does not require active replication to enter the nucleus. |
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*#Viral DNA is integrated into the host genome with viral integrase. |
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*#Viral DNA in the host genome is transcribed into mRNA and translated into viral proteins, including Gag. |
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*#Protease cleaves the Gag protein, which facilitates virion budding and release. |
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*Infection of lymphoid cells and lymph nodes, especially gut-associated lymphoid tissue (GALT) |
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**Infection therefore kills a large proportion of CD4 cells in the gut |
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*HIV enters from the mucosa to infect activated Langerhans macrophages, which then get to the local lymphoid tissue |
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===Epidemiology=== |
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* Two phases: initial viral attachment, fusion, reverse transcription, and integration; and the following lifetime of the viral infection |
|||
* Initial cellular infection |
|||
*# Binding or attachment of the virion gp120 Env surface protein to the CD4 receptor with CCR5 or CXCR4 coreceptor (on macrophage or T-cell, respectively). |
|||
*# Binding the receptor triggers a conformational change that exposes the fusion domain on gp41, which facilitates fusion and viral entry. The proceeding viral disassembly requires viral protein p24 to bind to cellular cyclophilin A. |
|||
*# In the cytoplasm, reverse transcriptase converts viral RNA into viral DNA. The RNA is degraded, then the complementary strand of DNA created. |
|||
*# The preintegration complex of double-stranded DNA is imported into the nucleus using viral Gag, viral protein R (Vpr), and integrase. Unlike other retroviruses, HIV does not require active replication to enter the nucleus. |
|||
* Infection of lymphoid cells and lymph nodes, especially gut-associated lymphoid tissue (GALT) |
|||
** Infection therefore kills a large proportion of CD4 cells in the gut |
|||
* HIV enters from the mucosa to infect activated Langerhans macrophages, which then get to the local lymphoid tissue |
|||
*63,000 Canadians living with HIV in 2016, of which 14% are unaware of their serostatus |
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== Epidemiology == |
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*Mode of transmission in Canada |
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**Sex among men who have sex with men (MSM) (52% of cases) |
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**People who inject drugs (17% of cases) |
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**Heterosexual sex (33% of cases) |
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*However, heterosexual sex is the most common mode of transmission worldwide |
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===Risk Factors=== |
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* 63,000 Canadians living with HIV in 2016 |
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* 14% don't know they have it |
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* Methods of acquisition in Canada |
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** MSM (52% of cases) |
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** People who inject drugs (17% of cases) |
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** Heterosexual sex (33% of cases) |
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*High-risk exposures |
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== Risk Factors == |
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**Men who have sex with men (MSM) |
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**Multiple partners |
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**Injection drug use |
|||
**Sex work |
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*Indigenous Canadians (2.7x higher incidence) |
|||
*African and Caribbean people (endemic countries) |
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*Prior [[sexually-transmitted infection]] |
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*Blood transfusion before 1983 or 84 |
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==Clinical Manifestations== |
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* High-risk exposures |
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** MSM |
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** Multiple partners |
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** Injection drug use |
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** Sex work |
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* Aboriginal Canadians (2.7x higher incidence) |
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* African and Caribbean people (endemic countries) |
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* Prior STIs |
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== |
===Stages=== |
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=== |
====CDC==== |
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*Developed by the CDC to provide some risk stratification for opportunistic infection |
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* Influenza-like illness |
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*Patients are classified based on the most advanced stage ever reached, and not reclassified based on response to therapy |
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* Rash |
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* ... |
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{| class="wikitable" |
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=== Chronic HIV === |
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!Stage |
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!Laboratory Evidence |
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!Clinical Evidence |
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|- |
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|0 |
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|negative/indeterminate HIV test within 180 days before first confirmed positive HIV test, or sequence of tests that demonstrate the presence of HIV-specific viral markers 0 to 180 days before or after antibody test that had a negative/indeterminate result |
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|no [[AIDS-defining illnesses]] |
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|- |
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|1 |
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|laboratory-confirmed HIV infection, with CD4 >500 or ≥29% |
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|no [[AIDS-defining illnesses]] |
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|- |
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|2 |
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|laboratory-confirmed HIV infection, with CD4 200-499 or 14-28% |
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|no [[AIDS-defining illnesses]] |
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|- |
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|3 |
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|laboratory-confirmed HIV infection, with CD4 <200 or <14% |
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|OR [[AIDS-defining illnesses]] |
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|- |
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|unknown |
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|laboratory confirmed HIV infection, but no information about CD4 count or percentage |
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|no [[AIDS-defining illnesses]] |
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|} |
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====WHO==== |
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* Fever |
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{| class="wikitable" |
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* Weight loss |
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!Clinical Stage |
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* Dyspnea, cough, hemoptysis |
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!Symptoms |
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* Dysphagia, diarrhea |
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!CD4 |
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* Anemia, neutropenia, thrombocytopenia |
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|- |
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* Metabolic derangements |
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|1 |
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* [Opportunistic infections](Complications/Opportunistic infections/Opportunistic infections.md) |
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|asymptomatic, or persistent generalized lymphadenopathy |
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|≥500 |
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|- |
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|2 |
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|unexplained weight loss <10%, recurrent respiratory tract infections, [[herpes zoster]], [[angular cheilitis]], recurrent oral ulcers, papular pruritic eruption, fungal nail infections, [[seborrheic dermatitis]] |
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|350-499 |
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|- |
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|3 |
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|unexplained weight loss >10%, unexplained diarrhea >1 month, unexplained fever >1 month, persistent oral candidiasis, [[oral hairy leukoplakia]], [[pulmonary tuberculosis]], severe bacterial infections, acute necrotizing ulcerative stomatisis, gingivitis, or periodontitis, unexplained anemia <80, unexplained neutropenia <0.5, unexplained thrombocytopenia <50 |
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|200-349 |
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|- |
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|4 |
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|HIV wasting syndrome, [[Pneumocystis jirovecii]], recurrent severe bacterial pneumonia, chronic herpes simplex infection >1 month, esophageal candidiasis, extrapulmonary tuberculosis, Kaposi sarcoma, CMV infection, CNS toxoplasmosis, HIV encephalopathy, extrapulmonary cryptococcosis, disseminated non-tuberculous mycobacteria, progressive multifocal leukoencephalopathy, chronic cryptosporidiosis or isosporiasis, disseminated endemic mycosis, CNS lymphoma, B-cell non-Hodgkin lymphoma, symptomatic HIV-associated nephropathy, symptomatic HIV-associated cardiomyopathy, recurrent bacteremia, invasive cervical carcinoma, atypical disseminated leishmaniasis |
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|<200 or <15% |
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|} |
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== |
===Acute HIV=== |
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*Incubation period [[Usual incubation period::2 to 6 weeks]] |
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* '''HIV serology''' |
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*Usually presents as an [[influenza]]- or [[mononucleosis]]-like illness, corresponding to very high viral load (in the millions) and acute decrease in CD4 |
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** Can test for HIV antibodies and p24 antigen |
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**Infectivity is highest due to the very high viremia |
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** Window period of 3-4 weeks exists before antibodies are positive, and is shortened to 2-3 weeks with antigen testing |
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*Most common symptoms include [[Has symptom::fever]], [[Has symptom::lymphadenopathy]], [[Causes::pharyngitis]], and [[Has symptom::rash]] |
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** If concern for acute seroconversion syndrome (within 2-4 weeks of exposure), may need to repeat serology |
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*Other common symptoms include [[Has symptom::myalgias]], [[Has symptom::arthralgias]], [[Has symptom::headache]], [[Has symptom::diarrhea]], [[Has symptom::oral ulcers]], [[Has symptom::leukopenia]], [[Has symptom::thrombocytopenia]], and mild [[Has symptom::hepatitis]] |
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** Standard testing in Ontario includes HIV 1+2 antigen/antibody ELISA screen, followed by confirmatory p24 antigen ELISA |
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*Can rarely cause [[encephalopathy]] or [[neuropathy]] |
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* '''HIV qualitative PCR''' |
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*Illness lasts 10 to 15 days, followed by recovery of CD4 and suppression of viral load over weeks to months |
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** Indicated in cases of suspected acute seroconversion (with negative serology), previous indeterminate antibody results, or a newborn of an HIV-infected mother |
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** More specific than quantitative PCR for viral load |
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===Chronic HIV=== |
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** Can be done from dried blood spot |
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** Generally only done for HIV-1 outside of a reference lab |
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*Following acute infection, there is a long latency period before development of overt symptoms and opportunistic diseases |
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*Progression from HIV infection to AIDS takes on average 10 years |
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**Speed of progression is proportional to viral load |
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*Some people progress quickly to AIDS in 5 years, and others are long-term nonprogressors that remain asymptomatic without treatment |
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**Non-progressors may have detectable viremia but normal CD4 counts, but with a CD4 count that eventually decreases |
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**Elite controllers are non-progressors that have no detectable viremia despite infection, and maintain CD4 counts |
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*Symptoms depend on severity of immunodeficiency; refer to WHO staging above for a long list of possible symptoms, but commonly include: |
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**Fevers |
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**Weight loss |
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**Dyspnea, cough, hemoptysis |
|||
**Dysphagia, diarrhea |
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**Anemia, neutropenia, thrombocytopenia |
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**Metabolic derangements |
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**[[Opportunistic infections in HIV|Opportunistic infections]] |
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*Direct effects of HIV infection include: |
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**Neuropsychiatric: HIV-associated neurocognitive disorders (must be differentiated from [[progressive multifocal leukoencephalopathy]] or other [[Opportunistic infections in HIV|opportunistic infections]]), neuropathy, radiculopathy (usually lumbosacral polyradiculopathy), myelopathy, HIV-associated retinopathy |
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**Cardiovascular: HIV-associated cardiomyopathy, early atherosclerosis |
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**Pulmonary: HIV-associated [[pulmonary hypertension]], possibly emphysema |
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**Gastrointestinal: HIV-induced enteropathy, possibly non-alcoholic fatty liver disease |
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**Renal: HIV-associated nephropathy |
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**Endocrine: impaired lipid and glucose metabolism, [[HIV wasting syndrome]], lipodystrophy, possibly hypogonadism and premature ovarian failure |
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**Musculoskeletal: myopathy, myositis |
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**Hematologic: anemia of chronic disease, possibly coagulopathy |
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**Dermatologic: possibly eosinophilic folliculitis |
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===Advanced HIV/AIDS=== |
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*Acquired immunodeficiency syndrome (AIDS) occurs when the cell-mediated immunodeficiency progresses to the point where opportunistic infections and malignancies occur ([[AIDS-defining illnesses]]) |
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*Medial survival if untreated is 12 to 18 months (38 to 40 months once CD4 counts drops below 200) |
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==Diagnosis== |
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*'''HIV serology''' |
|||
**Can test for HIV antibodies (usually combined IgM/IgG) and p24 antigen |
|||
**Window period of 3-4 weeks exists before antibodies are positive, and is shortened to 2-3 weeks with antigen testing (included in fourth-generation testing) |
|||
**If concern for acute seroconversion syndrome (within 2-4 weeks of exposure), may need to repeat serology |
|||
**Standard testing in Ontario includes HIV 1+2 antigen/antibody ELISA screen, followed by confirmatory p24 antigen ELISA |
|||
*'''HIV qualitative PCR''' |
|||
**Indicated in cases of suspected acute seroconversion (with negative serology), previous indeterminate antibody results, or a newborn of an HIV-infected mother |
|||
**More specific than quantitative PCR for viral load |
|||
**Can be done from dried blood spot |
|||
**Generally only done for HIV-1 outside of a reference lab |
|||
{| class="wikitable" |
{| class="wikitable" |
||
! |
!Ab/Ag!!Ab!!Ag!!RNA!!Interpretation |
||
|- |
|- |
||
| style="text-align:center;" |– |
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| – || || || || HIV negative, or window period if within 2-3 weeks of exposure |
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| |
|||
| |
|||
| |
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|HIV negative, or within serologic window period (2-3 weeks) |
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|- |
|- |
||
| style="text-align:center;" |– |
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| – || || || + || HIV positive (window period up to 2-3 weeks) |
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| |
|||
| |
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| style="text-align:center;" | + |
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|HIV positive, within the serologic window period (2-3 weeks) |
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|- |
|- |
||
| style="text-align:center;" | + |
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| + || + || || || HIV positive (following 3-4 week window period) |
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| style="text-align:center;" | + |
|||
| |
|||
| |
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|HIV positive, following a 3-4 week window period |
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|- |
|- |
||
| style="text-align:center;" | + |
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| + || – || + || || HIV positive (window period up to 3-4 weeks) |
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| style="text-align:center;" |– |
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| style="text-align:center;" | + |
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| |
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|HIV positive, within the serologic window period for antibodies (3-4 weeks) |
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|} |
|} |
||
== |
==Investigations== |
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*See [[Initial assessment for patients with HIV]] for baseline bloodwork |
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==Management== |
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* See [[First clinic visit for HIV]] for baseline bloodwork |
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===Initial management=== |
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*[[Initial assessment for patients with HIV]] |
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== Management == |
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*[[Single-tablet regimens for HIV]] |
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*[[HIV treatment]] |
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=== |
===Follow-up=== |
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* [[ |
*See also [[Routine follow-up for patients with HIV]] |
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*HIV viral load |
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* [[Single-tablet regimens for HIV]] |
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**Every 4 to 6 weeks until undetectable |
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* [[HIV treatment]] |
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**Then every 3 months until undetectable for 1 year |
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**Then every 6 months |
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*CD4 count |
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**Every 3 to 4 months until viral load undetectable and CD4 count >350 for 1 year |
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**Then every 6 months until viral load undetectable for at least 2 years and CD4 count > 500 |
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**Then stop monitoring routinely unless evidence of treatment failure |
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**Assess for failure if RNA level remains detectable at 24 weeks or if it increases to above 50 at any time |
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*Repeat RNA level within 4 weeks |
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=== |
=== Failure === |
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* Several types of failure: |
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* HIV viral load |
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** Clinical failure is the development of new or recurrent clinical events indicating severe immunodeficiency (WHO stage 4) after 6 months of antiretroviral therapy |
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** Every 4 to 6 weeks until undetectable |
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** Immunologic failure is CD4 count falling below baseline, or is persistently below 100 cells/mm<sup>3</sup> |
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** Then every 3 months until undetectable for 1 year |
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** Virologic failure is a viral load over 1000 copies/mL in two consecutive viral loads after 3 months of antiretroviral therapy |
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** Then every 6 months |
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*** May have "blips" of low-level viremia above the lower limit of the assay, but these blips do not constitute virologic failure |
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* CD4 count |
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* The differential for failure includes: |
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** Every 3 to 4 months until viral load undetectable and CD4 count >350 for 1 year |
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** Non-adherence |
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** Then every 6 months until viral load undetectable for at least 2 years and CD4 count > 500 |
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** Decreased absorption or altered metabolism, including from drug-drug interactions (e.g. proton pump inhibitors), mistimed medication, not taking with food (e.g. [[rilpivirine]]), taking with food, diarrhea or other GI illness that can decrease absorption |
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** Then stop monitoring routinely unless evidence of treatment failure |
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** [[Antiretroviral resistance in HIV|Drug resistance]] |
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** Assess for failure if RNA level remains detectable at 24 weeks or if it increases to above 50 at any time |
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* Repeat RNA level within 4 weeks |
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[[Category:HIV]] |
[[Category:HIV]] |
Latest revision as of 14:32, 22 October 2020
Background
- A chronic immunodeficiency resulting from infection with the human immunodeficiency virus (HIV)
- Acquired immune deficiency syndrome (AIDS) is a severe form of HIV characterized by low CD4 count resulting in characteristic infections
Microbiology
- A member of the Retroviridae family
- Clades or subtypes:
- HIV-1: by far the most common species worldwide
- M group
- Clade A: common in East Africa
- Clade B: is common in Canada, Americas, Europe
- M group
- HIV-2: essentially confined to West Africa and certain parts of southern Europe and Asia
- HIV-1: by far the most common species worldwide
Life Cycle
- Two phases: initial viral attachment, fusion, reverse transcription, and integration; and the following lifetime of the viral infection
- Initial cellular infection
- Binding or attachment of the virion gp120 Env surface protein to the CD4 receptor with CCR5 or CXCR4 coreceptor (on macrophage or T-cell, respectively).
- Binding the receptor triggers a conformational change that exposes the fusion domain on gp41, which facilitates fusion and viral entry. The proceeding viral disassembly requires viral protein p24 to bind to cellular cyclophilin A.
- In the cytoplasm, reverse transcriptase converts viral RNA into viral DNA. The RNA is degraded, then the complementary strand of DNA created.
- The preintegration complex of double-stranded DNA is imported into the nucleus using viral Gag, viral protein R (Vpr), and integrase. Unlike other retroviruses, HIV does not require active replication to enter the nucleus.
- Viral DNA is integrated into the host genome with viral integrase.
- Viral DNA in the host genome is transcribed into mRNA and translated into viral proteins, including Gag.
- Protease cleaves the Gag protein, which facilitates virion budding and release.
- Infection of lymphoid cells and lymph nodes, especially gut-associated lymphoid tissue (GALT)
- Infection therefore kills a large proportion of CD4 cells in the gut
- HIV enters from the mucosa to infect activated Langerhans macrophages, which then get to the local lymphoid tissue
Epidemiology
- 63,000 Canadians living with HIV in 2016, of which 14% are unaware of their serostatus
- Mode of transmission in Canada
- Sex among men who have sex with men (MSM) (52% of cases)
- People who inject drugs (17% of cases)
- Heterosexual sex (33% of cases)
- However, heterosexual sex is the most common mode of transmission worldwide
Risk Factors
- High-risk exposures
- Men who have sex with men (MSM)
- Multiple partners
- Injection drug use
- Sex work
- Indigenous Canadians (2.7x higher incidence)
- African and Caribbean people (endemic countries)
- Prior sexually-transmitted infection
- Blood transfusion before 1983 or 84
Clinical Manifestations
Stages
CDC
- Developed by the CDC to provide some risk stratification for opportunistic infection
- Patients are classified based on the most advanced stage ever reached, and not reclassified based on response to therapy
Stage | Laboratory Evidence | Clinical Evidence |
---|---|---|
0 | negative/indeterminate HIV test within 180 days before first confirmed positive HIV test, or sequence of tests that demonstrate the presence of HIV-specific viral markers 0 to 180 days before or after antibody test that had a negative/indeterminate result | no AIDS-defining illnesses |
1 | laboratory-confirmed HIV infection, with CD4 >500 or ≥29% | no AIDS-defining illnesses |
2 | laboratory-confirmed HIV infection, with CD4 200-499 or 14-28% | no AIDS-defining illnesses |
3 | laboratory-confirmed HIV infection, with CD4 <200 or <14% | OR AIDS-defining illnesses |
unknown | laboratory confirmed HIV infection, but no information about CD4 count or percentage | no AIDS-defining illnesses |
WHO
Clinical Stage | Symptoms | CD4 |
---|---|---|
1 | asymptomatic, or persistent generalized lymphadenopathy | ≥500 |
2 | unexplained weight loss <10%, recurrent respiratory tract infections, herpes zoster, angular cheilitis, recurrent oral ulcers, papular pruritic eruption, fungal nail infections, seborrheic dermatitis | 350-499 |
3 | unexplained weight loss >10%, unexplained diarrhea >1 month, unexplained fever >1 month, persistent oral candidiasis, oral hairy leukoplakia, pulmonary tuberculosis, severe bacterial infections, acute necrotizing ulcerative stomatisis, gingivitis, or periodontitis, unexplained anemia <80, unexplained neutropenia <0.5, unexplained thrombocytopenia <50 | 200-349 |
4 | HIV wasting syndrome, Pneumocystis jirovecii, recurrent severe bacterial pneumonia, chronic herpes simplex infection >1 month, esophageal candidiasis, extrapulmonary tuberculosis, Kaposi sarcoma, CMV infection, CNS toxoplasmosis, HIV encephalopathy, extrapulmonary cryptococcosis, disseminated non-tuberculous mycobacteria, progressive multifocal leukoencephalopathy, chronic cryptosporidiosis or isosporiasis, disseminated endemic mycosis, CNS lymphoma, B-cell non-Hodgkin lymphoma, symptomatic HIV-associated nephropathy, symptomatic HIV-associated cardiomyopathy, recurrent bacteremia, invasive cervical carcinoma, atypical disseminated leishmaniasis | <200 or <15% |
Acute HIV
- Incubation period 2 to 6 weeks
- Usually presents as an influenza- or mononucleosis-like illness, corresponding to very high viral load (in the millions) and acute decrease in CD4
- Infectivity is highest due to the very high viremia
- Most common symptoms include fever, lymphadenopathy, pharyngitis, and rash
- Other common symptoms include myalgias, arthralgias, headache, diarrhea, oral ulcers, leukopenia, thrombocytopenia, and mild hepatitis
- Can rarely cause encephalopathy or neuropathy
- Illness lasts 10 to 15 days, followed by recovery of CD4 and suppression of viral load over weeks to months
Chronic HIV
- Following acute infection, there is a long latency period before development of overt symptoms and opportunistic diseases
- Progression from HIV infection to AIDS takes on average 10 years
- Speed of progression is proportional to viral load
- Some people progress quickly to AIDS in 5 years, and others are long-term nonprogressors that remain asymptomatic without treatment
- Non-progressors may have detectable viremia but normal CD4 counts, but with a CD4 count that eventually decreases
- Elite controllers are non-progressors that have no detectable viremia despite infection, and maintain CD4 counts
- Symptoms depend on severity of immunodeficiency; refer to WHO staging above for a long list of possible symptoms, but commonly include:
- Fevers
- Weight loss
- Dyspnea, cough, hemoptysis
- Dysphagia, diarrhea
- Anemia, neutropenia, thrombocytopenia
- Metabolic derangements
- Opportunistic infections
- Direct effects of HIV infection include:
- Neuropsychiatric: HIV-associated neurocognitive disorders (must be differentiated from progressive multifocal leukoencephalopathy or other opportunistic infections), neuropathy, radiculopathy (usually lumbosacral polyradiculopathy), myelopathy, HIV-associated retinopathy
- Cardiovascular: HIV-associated cardiomyopathy, early atherosclerosis
- Pulmonary: HIV-associated pulmonary hypertension, possibly emphysema
- Gastrointestinal: HIV-induced enteropathy, possibly non-alcoholic fatty liver disease
- Renal: HIV-associated nephropathy
- Endocrine: impaired lipid and glucose metabolism, HIV wasting syndrome, lipodystrophy, possibly hypogonadism and premature ovarian failure
- Musculoskeletal: myopathy, myositis
- Hematologic: anemia of chronic disease, possibly coagulopathy
- Dermatologic: possibly eosinophilic folliculitis
Advanced HIV/AIDS
- Acquired immunodeficiency syndrome (AIDS) occurs when the cell-mediated immunodeficiency progresses to the point where opportunistic infections and malignancies occur (AIDS-defining illnesses)
- Medial survival if untreated is 12 to 18 months (38 to 40 months once CD4 counts drops below 200)
Diagnosis
- HIV serology
- Can test for HIV antibodies (usually combined IgM/IgG) and p24 antigen
- Window period of 3-4 weeks exists before antibodies are positive, and is shortened to 2-3 weeks with antigen testing (included in fourth-generation testing)
- If concern for acute seroconversion syndrome (within 2-4 weeks of exposure), may need to repeat serology
- Standard testing in Ontario includes HIV 1+2 antigen/antibody ELISA screen, followed by confirmatory p24 antigen ELISA
- HIV qualitative PCR
- Indicated in cases of suspected acute seroconversion (with negative serology), previous indeterminate antibody results, or a newborn of an HIV-infected mother
- More specific than quantitative PCR for viral load
- Can be done from dried blood spot
- Generally only done for HIV-1 outside of a reference lab
Ab/Ag | Ab | Ag | RNA | Interpretation |
---|---|---|---|---|
– | HIV negative, or within serologic window period (2-3 weeks) | |||
– | + | HIV positive, within the serologic window period (2-3 weeks) | ||
+ | + | HIV positive, following a 3-4 week window period | ||
+ | – | + | HIV positive, within the serologic window period for antibodies (3-4 weeks) |
Investigations
- See Initial assessment for patients with HIV for baseline bloodwork
Management
Initial management
Follow-up
- See also Routine follow-up for patients with HIV
- HIV viral load
- Every 4 to 6 weeks until undetectable
- Then every 3 months until undetectable for 1 year
- Then every 6 months
- CD4 count
- Every 3 to 4 months until viral load undetectable and CD4 count >350 for 1 year
- Then every 6 months until viral load undetectable for at least 2 years and CD4 count > 500
- Then stop monitoring routinely unless evidence of treatment failure
- Assess for failure if RNA level remains detectable at 24 weeks or if it increases to above 50 at any time
- Repeat RNA level within 4 weeks
Failure
- Several types of failure:
- Clinical failure is the development of new or recurrent clinical events indicating severe immunodeficiency (WHO stage 4) after 6 months of antiretroviral therapy
- Immunologic failure is CD4 count falling below baseline, or is persistently below 100 cells/mm3
- Virologic failure is a viral load over 1000 copies/mL in two consecutive viral loads after 3 months of antiretroviral therapy
- May have "blips" of low-level viremia above the lower limit of the assay, but these blips do not constitute virologic failure
- The differential for failure includes:
- Non-adherence
- Decreased absorption or altered metabolism, including from drug-drug interactions (e.g. proton pump inhibitors), mistimed medication, not taking with food (e.g. rilpivirine), taking with food, diarrhea or other GI illness that can decrease absorption
- Drug resistance