HIV AIDS medical therapy: Difference between revisions

{{CMG}}

The primary goal of antiretroviral therapy (ART) is to reduce HIV-associated [[morbidity]] and [[mortality]]. This goal is best accomplished by using effective ART to maximally inhibit HIV replication, as defined by achieving and maintaining [[plasma]] HIV [[RNA]] ([[viral load]]) below levels detectable by commercially available [[assay]]s. Durable viral suppression improves immune function and quality of life, lowers the risk of both AIDS-defining and non-AIDS-defining complications, and prolongs life. Based on emerging evidence, additional benefits of ART include a reduction in HIV-associated [[inflammation]] and possibly its associated complications.

# [[Non-nucleoside reverse transcriptase inhibitors]] (NNRTIs).

# [[Nucleoside reverse transcriptase inhibitors]] (NRTIs).

# [[Protease inhibitors]] (PIs).

# [[Fusion inhibitor]]s.

# [[CCR5]] antagonists.

# [[Integrase inhibitors]].

==Chapter Outline==

*[[AIDS medical therapy#Goals of Therapy|Goals of Therapy]]

*[[AIDS medical therapy#Anti Retroviral Therapy (ART)|Anti Retroviral Therapy]]

:[[AIDS medical therapy#Guidelines for Initiation of ART|Guidelines for Initiation of ART]] | [[AIDS medical therapy#Indications|Indications]] | [[AIDS medical therapy#Selection of the Regimen|Selection of the Regimen]] | [[AIDS medical therapy#Treatment-naive Patients|Treatment-naive Patients]] | [[AIDS medical therapy#Treatment-experienced patients|Treatment-experienced Patients]] | [[AIDS medical therapy#Initial HIV Therapy|Initial HIV Therapy]] | [[AIDS medical therapy#Highly Active Anti-Retroviral Therapy|Highly Active Anti-Retroviral Therapy]] | [[AIDS medical therapy#Special Considerations|Special Considerations]] | [[AIDS medical therapy#HIV in Children|HIV in Children]]

* [[AIDS medical therapy#Treatment Adherence|Treatment Adherence]]

: [[AIDS medical therapy#Difficulty in Adherence|Difficulty in Adherence]] | [[AIDS medical therapy#Importance of Adherence|Importance of Adherence]]

: [[AIDS medical therapy#Visit Frequency|Visit Frequency]] | [[AIDS medical therapy#General Laboratory Investigations|General Laboratory Investigations]] | [[AIDS medical therapy#Virologic Response|Virologic Response]] | [[AIDS medical therapy#Virologic Failure|Virologic Failure]] | [[AIDS medical therapy#Viral Blips|Viral Blips]]

* [[AIDS medical therapy#Indications for Modification of Therapy|Indications for Modification of Therapy]]

==Goals of Therapy==

DHHS ART Guidelines present the following goals for therapy:  

* Durable suppression of HIV [[viral load]] ( to <50 cells/mL ).

* Restoration of normal CD4 cell count.

* Prevention of transmission of the disease.

* Prevention of building of [[drug resistance]].

* Improvement in quality of life of the patient.

Uncontrolled [[viremia]] causes [[inflammation]] and immune activation, which has an overall effect on [[cardiovascular]], [[renal]] and [[hepatic]] systems. Controlling viremia also controls these effects.

==Anti Retroviral Therapy (ART)==

===Guidelines for initiation of ART===

<center>

{| border="1"

|+

|

| Year

| AIDS/Symptoms

| CD4 <200

| CD4 200-350

| CD4 350-500

| CD4 >500

| DHHS [http://aidsinfo.nih.gov/contentfiles/AdultandAdolescentGL.pdf]

| 2011

| Yes

| Yes

| Yes

| Yes

| Yes (optional)

| IAS-USA<ref name="pmid20639566">{{cite journal |author=Thompson MA, Aberg JA, Cahn P, Montaner JS, Rizzardini G, Telenti A, Gatell JM, Günthard HF, Hammer SM, Hirsch MS, Jacobsen DM, Reiss P, Richman DD, Volberding PA, Yeni P, Schooley RT |title=Antiretroviral treatment of adult HIV infection: 2010 recommendations of the International AIDS Society-USA panel |journal=JAMA |volume=304 |issue=3 |pages=321–33 |year=2010 |month=July |pmid=20639566 |doi=10.1001/jama.2010.1004 |url=http://jama.ama-assn.org/cgi/pmidlookup?view=long&pmid=20639566 |accessdate=2012-03-08}}</ref>

| UK

| 2008

| EACS<ref name="pmid18257769">{{cite journal |author=Clumeck N, Pozniak A, Raffi F |title=European AIDS Clinical Society (EACS) guidelines for the clinical management and treatment of HIV-infected adults |journal=HIV Med. |volume=9 |issue=2 |pages=65–71 |year=2008 |month=February |pmid=18257769 |doi=10.1111/j.1468-1293.2007.00533.x |url=http://onlinelibrary.wiley.com/resolve/openurl?genre=article&sid=nlm:pubmed&issn=1464-2662&date=2008&volume=9&issue=2&spage=65 |accessdate=2012-03-08}}</ref>

| WHO [[http://www.who.int/hiv/pub/guidelines/artadultguidelines.pdf]]

| 2010

| No

| No

===Indications===

The DHHS guidelines currently recommend the follwing:

{|border="1" align="center" style="background:white"

| bgcolor="white" |'''Symptoms'''

| bgcolor="white" |'''Treatment'''

| Asymptomatic

| <500

| Treatment should be offered.

| Asymptomatic

| >500

| Treatment is optional.

| [[AIDS history and symptoms#History and Symptoms|Symptomatic]]

| Any value

| Treatment should be initiated.<ref name="pmid20639566">{{cite journal |author=Thompson MA, Aberg JA, Cahn P, Montaner JS, Rizzardini G, Telenti A, Gatell JM, Günthard HF, Hammer SM, Hirsch MS, Jacobsen DM, Reiss P, Richman DD, Volberding PA, Yeni P, Schooley RT |title=Antiretroviral treatment of adult HIV infection: 2010 recommendations of the International AIDS Society-USA panel |journal=JAMA |volume=304 |issue=3 |pages=321–33 |year=2010 |month=July |pmid=20639566 |doi=10.1001/jama.2010.1004 |url=http://jama.ama-assn.org/cgi/pmidlookup?view=long&pmid=20639566 |accessdate=2012-02-15}}</ref>

===Selection of the Regimen===

====A. US Department of Health and Human Services (DHHS)====

DHHS have published guidelines for initial ART based on data from randomized controlled trials.  Current optimal HAART options consist of combinations (or "cocktails") consisting of at least three drugs belonging to at least two types, or "classes," of [[antiretroviral]] agents.

Typical regimens consist of:

* Two [[nucleoside analogue reverse transcriptase inhibitor]]s (NARTIs or NRTIs) '''PLUS'''

* Either a [[protease inhibitor (pharmacology)|protease inhibitor]] or a [[non-nucleoside reverse transcriptase inhibitor]] (NNRTI).

* An [[NNRTI]], [[efavirenz]] plus 2 [[NRTI]]s '''OR'''

* A boosted PI: [[atazanavir]] (ATV/r) once daily or [[darunavir]] (DRV/r) once daily plus 2 NRTIs '''OR'''

* An integrase inhibitor, [[raltegravir]] (400 mg twice daily) with 2 NRTIs.

The recommended NRTI coformulation is [[tenofovir]]/[[emtricitabine]] (TDF/FTC) in all of the above combinations.

In treatment-naive patients, four drug regimen is not found to be more efficacious than three-drug regimens and is associated with more adverse events.<ref name="pmid14668456">{{cite journal |author=Shafer RW, Smeaton LM, Robbins GK, De Gruttola V, Snyder SW, D'Aquila RT, Johnson VA, Morse GD, Nokta MA, Martinez AI, Gripshover BM, Kaul P, Haubrich R, Swingle M, McCarty SD, Vella S, Hirsch MS, Merigan TC |title=Comparison of four-drug regimens and pairs of sequential three-drug regimens as initial therapy for HIV-1 infection |journal=N. Engl. J. Med. |volume=349 |issue=24 |pages=2304–15 |year=2003 |month=December |pmid=14668456 |doi=10.1056/NEJMoa030265 |url=http://dx.doi.org/10.1056/NEJMoa030265 |accessdate=2012-02-16}}</ref><ref name="pmid20735258">{{cite journal |author=Puls RL, Srasuebkul P, Petoumenos K, Boesecke C, Duncombe C, Belloso WH, Molina JM, Li L, Avihingsanon A, Gazzard B, Cooper DA, Emery S |title=Efavirenz versus boosted atazanavir or zidovudine and abacavir in antiretroviral treatment-naive, HIV-infected subjects: week 48 data from the Altair study |journal=Clin. Infect. Dis. |volume=51 |issue=7 |pages=855–64 |year=2010 |month=October |pmid=20735258 |doi=10.1086/656363 |url=http://www.cid.oxfordjournals.org/cgi/pmidlookup?view=long&pmid=20735258 |accessdate=2012-02-16}}</ref>

====B. International AIDS Society-USA (IAS-USA) Guidelines ====

In agreement with the DHHS guidelines mentioned above, IAS-USA recommend the following:<ref name="pmid20639566">{{cite journal |author=Thompson MA, Aberg JA, Cahn P, Montaner JS, Rizzardini G, Telenti A, Gatell JM, Günthard HF, Hammer SM, Hirsch MS, Jacobsen DM, Reiss P, Richman DD, Volberding PA, Yeni P, Schooley RT |title=Antiretroviral treatment of adult HIV infection: 2010 recommendations of the International AIDS Society-USA panel |journal=JAMA |volume=304 |issue=3 |pages=321–33 |year=2010 |month=July |pmid=20639566 |doi=10.1001/jama.2010.1004 |url=http://jama.ama-assn.org/cgi/pmidlookup?view=long&pmid=20639566 |accessdate=2012-02-21}}</ref>

The DHHS Guidelines recommend that therapy should be initiated in the following patient populations:

* Patients with history of an AIDS-defining illness or with a [[CD4]] count of less than 350/µL.

* Pregnant women with HIV [[infection]].

* Patients with HIV and [[hepatitis B virus]] (HBV) coinfection who require treatment for HBV infection.

[[Fusion inhibitor]]s (eg, [[enfuvirtide]]) are not approved for treatment-naive patients.

Treatment failure is defined by the following factors:

* '''Virologic failure''': which is defined as suboptimal viral suppression or loss of suppression (>50 HIV-1 RNA copies/mL).

* '''Immunologic failure ''': which is defined as failure to achieve or maintain [[CD4]] cell count recovery despite effective viral suppression.

* Development of new [[opportunistic infection]]s or [[neoplasm]]s despite apparent CD4 count recovery.

===Initial HIV therapy===

NNRTI, PI, or integrase inhibitor-based regimen in combination with dual NRTIs is considered as an initial HIV therapy. Currently, CCR5 inhibitors are not  recommended due to lack of sufficient published data.  The particular choice of agent depends on the following factors:

*Current treatment for HIV infection consists of [[highly active antiretroviral therapy]], or HAART.<ref name=DhhsHivTreatment>{{

| publisher=Department of Health and Human Services

| date=February 2006

| url=http://hab.hrsa.gov/tools/HIVpocketguide/PktGARTtables.htm

| title=A Pocket Guide to Adult HIV/AIDS Treatment February 2006 edition

| accessdate = 2006-09-01

}}</ref> This has been highly beneficial to many HIV-infected individuals since its introduction in 1996 when the protease inhibitor-based HAART initially became available. [[Image:Abacavir (Ziagen) 300mg.jpg|left|thumb|100px|''[[Abacavir]]'' – a nucleoside analog reverse transcriptase inhibitors (NARTIs or NRTIs)]]

*In developed countries where HAART is available, doctors assess the [[viral load]], rapidity in CD4 decline, and patient readiness while deciding when to recommend initiating treatment.<ref name=2005DhhsHivTreatment>{{

| publisher=Department of Health and Human Services Panel on Clinical Practices for Treatment of HIV Infection

| date=2005-10-06

| url=http://aidsinfo.nih.gov/ContentFiles/AdultandAdolescentGL.pdf

| title=Guidelines for the Use of Antiretroviral Agents in HIV-1-Infected Adults and Adolescents

| format= PDF

| accessdate = 2006-01-17

}}</ref>

*In the absence of HAART, progression from HIV infection to AIDS occurs at a median of between nine to ten years and the median survival time after developing AIDS is only 9.2&nbsp;months.  

| author=Tassie JM, Grabar S, Lancar R, Deloumeaux J, Bentata M, Costagliola D and the Clinical Epidemiology Group from the French Hospital Database on HIV

}}</ref> This average reflects the fact that for some patients &ndash; and in many clinical cohorts this may be more than fifty percent of patients &ndash; HAART achieves far less than optimal results. This is due to a variety of reasons such as medication intolerance/side effects, prior ineffective antiretroviral therapy and infection with a drug-resistant strain of HIV.

| author=Becker SL, Dezii CM, Burtcel B, Kawabata H, Hodder S. | title=Young HIV-infected adults are at greater risk for medication nonadherence | journal=MedGenMed. | year=2002 | pages=21 | volume=4| issue=3 | pmid=12466764

}}</ref><ref name=Saitoh>{{

| author=Saitoh A, Hull AD, Franklin P, Spector SA

| title=Myelomeningocele in an infant with intrauterine exposure to efavirenz

| journal=J. Perinatol. | year=2005 | pages=555&ndash;556 | volume=25 | issue=8

| pmid=16047034 | doi=10.1038/sj.jp.7211343

}}</ref>

* '''Side-Effect of HAART:''' Treatment optimism after the initial successes of HAART likely affected the subsequent dynamics of HIV because these favorable treatment outcomes led some persons to increase their high-risk behavior.

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}}</ref> Moreover, it would take more than the lifetime of an individual to be cleared of HIV infection using HAART.<ref name=blankson>{{

 

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}}</ref> Despite this, many HIV-infected individuals have experienced remarkable improvements in their general health and quality of life, which has led to the plummeting of HIV-associated morbidity and mortality.<ref name=Pallelal>{{

 

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Because HIV disease progression in children is more rapid than in adults, and laboratory parameters are less predictive of risk for disease progression, particularly for young infants, treatment recommendations are more aggressive for children than for adults.<ref name=2005dhhsHivChildren>{{

cite web

Adherence is taking the correct dose of each anti-HIV medication at the correct time and exactly as prescribed. Adherence is very important for successful HIV treatment. The reasons for non-adherence and non-persistence with HAART are varied and overlapping. Major psychosocial issues, such as poor access to medical care, inadequate social supports, psychiatric disease and drug abuse contribute to non-adherence. The complexity of these HAART regimens, whether due to pill number, dosing frequency, meal restrictions or other issues, along with side effects that create intentional non-adherence, also has a weighty impact.<ref name=Nieuwkerk>{{

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===Difficulty in adherence===

There are several reasons why adhering to an HIV treatment regimen can be diicult. Most treatment regimens involve taking several pills every day with or without food, or before or after other medications. Other factors that can make treatment adherence diicult include:  

 

 

Skipping medications makes it easier for drug resistance to develop. HIV can develop resistance to the anti-HIV medications in a person’s current regimen or to other, similar anti-HIV medications not yet taken, limiting options for successful HIV treatment. And drug-resistant strains of HIV can be transmitted to others, too. Although there are many diferent anti-HIV medications and treatment regimens, studies show that a person’s first regimen ofers the best chance for long-term treatment success. Adhering to the regimen from the start will help ensure that the HIV treatment is successful.

A patient monitoring system is the backbone of clinical care, treatment and prevention by the clinical team caring for groups of patients.

===Visit Frequency===

Patients who are started on ART should generally have follow-up within one to two weeks. Patient should be asked about the following:

* [[AIDS primary prevention#Prevention of sexual transmission of HIV|Prevention of transmission]].

Visit frequency of patients who are clinically stable on their ART regimen, can be decrease to every three months.

The following lab tests are adviced at baseline and at scheduled follow-up:

 

More frequent testing is indicated in the following conditions:

* If mild or moderate abnormalities are detected and the medication is continued.  

* Depending on the drug prescribed

** In patients on [[nevirapine]], some experts recommend monitoring at 0, 2, 4, 8, 12 weeks and then every 3 months.

** Women in childbearing age-group, should have a pregnancy test, before initiation of potential teratogenic drugs like [[efavirenz]].

** In patients taking [[zidovudine]], hematologic monitoring is important as the drug causes [[bone marrow suppression]].

**In patients taking [[tenofovir]], which can cause [[renal insufficiency]], monitoring of [[creatinine]] and [[urinalysis]] every six months is necessary.<ref name="pmid18171278">{{cite journal |author=Szczech LA |title=Tenofovir nephrotoxicity: focusing research questions and putting them into clinical context |journal=J. Infect. Dis. |volume=197 |issue=1 |pages=7–9 |year=2008 |month=January |pmid=18171278 |doi=10.1086/524091 |url=http://www.jid.oxfordjournals.org/cgi/pmidlookup?view=long&pmid=18171278 |accessdate=2012-02-18}}</ref>

The most reliable indicator of response to ART is plasma [[HIV structure and genome|HIV RNA]] and should be measured in all patients at baseline and regularly during therapy.<ref name="pmid10853978">{{cite journal |author=Thiébaut R, Morlat P, Jacqmin-Gadda H, Neau D, Mercié P, Dabis F, Chêne G |title=Clinical progression of HIV-1 infection according to the viral response during the first year of antiretroviral treatment. Groupe d'Epidémiologie du SIDA en Aquitaine (GECSA) |journal=AIDS |volume=14 |issue=8 |pages=971–8 |year=2000 |month=May |pmid=10853978 |doi= |url=http://meta.wkhealth.com/pt/pt-core/template-journal/lwwgateway/media/landingpage.htm?issn=0269-9370&volume=14&issue=8&spage=971 |accessdate=2012-02-19}}</ref><ref name="pmid9182469">{{cite journal |author=Hughes MD, Johnson VA, Hirsch MS, Bremer JW, Elbeik T, Erice A, Kuritzkes DR, Scott WA, Spector SA, Basgoz N, Fischl MA, D'Aquila RT |title=Monitoring plasma HIV-1 RNA levels in addition to CD4+ lymphocyte count improves assessment of antiretroviral therapeutic response. ACTG 241 Protocol Virology Substudy Team |journal=Ann. Intern. Med. |volume=126 |issue=12 |pages=929–38 |year=1997 |month=June |pmid=9182469 |doi= |url= |accessdate=2012-02-19}}</ref>  It is thus useful in predicting clinical progression.

{|border="1" align="center" style="background:white"

|-

| bgcolor="white" |''' Time '''

| bgcolor="white" |'''Expected decrease in Viral load'''

| 1 week

| decrease by 0.75 to 1 log10 copies/mL

| 1 month  

| decrease by 1.5 to 2 log10 copies/mL to <5000 copies/mL .

| 2 to 4 months.  

| <500 copies/mL  

| 4 to 6 months.

| < 50 copies/mL.

 

 

===Virologic failure===

#Drug resistance.

===Viral blips===  

It refer to an isolated low-level of detectable HIV RNA (>50 to 500 copies/mL) that occurs during long-term monitoring on a stable ART regimen.<ref name="pmid16206110">{{cite journal |author=Sungkanuparph S, Overton ET, Seyfried W, Groger RK, Fraser VJ, Powderly WG |title=Intermittent episodes of detectable HIV viremia in patients receiving nonnucleoside reverse-transcriptase inhibitor-based or protease inhibitor-based highly active antiretroviral therapy regimens are equivalent in incidence and prognosis |journal=Clin. Infect. Dis. |volume=41 |issue=9 |pages=1326–32 |year=2005 |month=November |pmid=16206110 |doi=10.1086/496985 |url=http://www.cid.oxfordjournals.org/cgi/pmidlookup?view=long&pmid=16206110 |accessdate=2012-02-21}}</ref>

 

 

 

Various forms of [[alternative medicine]] have been used to treat symptoms or alter the course of the disease.<ref name=Saltmarsh>{{

 

 

 

 

 

 

 

 

 

 

* ritonavir-boosted atazanavir + tenofovir/emtricitabine (ATV/r + TDF/FTC) ('''AI''')

* ritonavir-boosted darunavir + tenofovir/emtricitabine (DRV/r + TDF/FTC) ('''AI''')

* Selection of a regimen should be individualized on the basis of virologic efficacy, toxicity, pill burden, dosing frequency, drug-drug interaction potential, resistance testing results, and comorbid conditions.

* Evaluation of virologic failure should include an assessment of the severity of the patient’s HIV disease, ART history, use of concomitant medications with consideration of adverse drug interactions with ARV agents, HIV RNA and CD4 T-cell count trends over time, and prior drug-resistance testing results.

* The goal of treatment for ARV-experienced patients with drug resistance who are experiencing virologic failure is to reestablish virologic suppression (e.g., HIV RNA <48 copies/mL) ('''AI''').

* Discontinuing or briefly interrupting therapy in a patient with viremia may lead to a rapid increase in HIV RNA and a decrease in CD4 cell count and increases the risk of clinical progression. Therefore, this strategy is '''not''' recommended ('''AI''').

* Therapy should also be considered optional for patients with HIV seroconversion in the previous 6 months ('''CIII''').

* If the clinician and patient elect to treat acute HIV infection, treatment should be implemented with the goal of suppressing plasma HIV RNA to below detectable levels ('''AIII''').

* If the decision is made to initiate therapy in a person with acute HIV infection, genotypic resistance testing at baseline will be helpful in guiding the selection of an ARV regimen that can provide the optimal virologic response; this strategy is therefore recommended ('''AIII'''). If therapy is deferred, genotypic resistance testing should still be performed because the result may be useful in optimizing the virologic response when therapy is ultimately initiated ('''AIII''').

* Because clinically significant resistance to protease inhibitors (PIs) is less common than resistance to nonnucleoside reverse transcriptase inhibitors (NNRTIs) in antiretroviral therapy (ART)-naive persons who harbor drug-resistant virus, a ritonavir (RTV)-boosted PI-based regimen should be used if therapy is initiated before drug resistance test results are available ('''AIII''').

*Women taking antiretroviral (ARV) drugs that have significant pharmacokinetic interactions with oral contraceptives should use an additional or alternative contraceptive method to prevent unintended pregnancy ('''AIII''').

*In pregnant women, an additional goal of therapy is prevention of perinatal transmission of HIV, with a goal of maximal viral suppression to reduce the risk of transmission of HIV to the fetus and newborn ('''AI''').

* Use of efavirenz (EFV) should be avoided in a pregnant woman during the first trimester or in a woman who desires to become pregnant or who does not or cannot use effective and consistent contraception ('''AIII''').

* ART-associated adverse events may occur more frequently in older HIV-infected adults than in younger HIV-infected individuals. Therefore, the bone, kidney, metabolic, cardiovascular, and liver health of older HIV-infected adults should be monitored closely.

[[AIDS medical therapy#top|Back to the top of the page]]

==Related Chapters==

*[[HIV#Treatment|HIV Treatment]]

*[[Antiretroviral drug]]

*[[Antiretroviral therapy in pregnancy]]

*[[Immune reconstitution inflammatory syndrome]]