Temporary Disabled. :) please Go back Starting, monitoring & switching HIV treatment www.fgks.org » Address: [go: up one dir, main page] Include Form Remove Scripts Accept Cookies Show Images Show Referer Rotate13 Base64 Strip Meta Strip Title Session Cookies International HIV & AIDS charity DonateFundraising About Us Our Partners Help & Advice Contact Us Facebook Linked in Twitter Newsletter Copyright © AVERT skip to menu Starting, monitoring & switching HIV treatment Contents Starting HIV treatment Choosing the best combination Monitoring HIV treatment Switching treatment HIV transmission and antiretroviral drugs Deciding when to start antiretroviral treatment depends on the stage of HIV infection which is determined through clinical tests. Once it is decided that an HIV positive patient should start treatment, a variety of factors must be considered when choosing the right combination of drugs for that person. After a person starts treatment, the effectiveness of their treatment must be monitored so that if necessary, the treatment regimen can be switched. This page discusses these main issues surrounding starting, monitoring and switching HIV treatment in more detail. back to top Starting HIV treatment There is no proven ‘right’ time to start antiretroviral drug treatment for HIV and AIDS. When a person is diagnosed with HIV, they will not necessarily need to start treatment immediately. Starting treatment depends on the stage of HIV infection; most guidelines recommend not starting until the advanced stages of HIV infection because it is an important decision with long-term consequences. The decision also depends on the person; children and pregnant women for example are generally advised to start treatment at an earlier stage compared to other people infected with HIV. In order to decide whether or not an HIV positive patient should start treatment, clinical tests need to be carried out. These tests determine the stage of HIV infection and the individual patient's readiness for drug treatment, which may depend on a variety of factors such as the patient’s medical history. The CD4 test Usually, the CD4 test is used to determine when a person should start treatment. CD4 testing at Saint Francis Hospital in Katete, Zambia HIV attacks a type of immune system cell called the T-helper cell. The T-helper cell plays an essential part in the immune system by helping to co-ordinate all the other cells to fight illnesses. HIV damages and destroys T-helper cells; as a result, there are fewer cells available to help the immune system. A major reduction in the number of T-helper cells can have a serious effect on the immune system. A CD4 test measures the number of T-helper cells (in a cubic millimetre of blood) which is known as a CD4 count. Someone who is not infected with HIV normally has between 500 and 1200 cells/mm3. In a person infected with HIV, the CD4 count often declines over a number of years. HIV drug treatment is generally recommended when the CD4 test shows fewer than 350 cells/mm3. World Health Organization (WHO) 2010 guidelines recommend starting treatment for all patients with CD4 counts of <350 cells/mm3 in all countries.1 Although most resource-limited countries aim to follow these guidelines, a number still observe the WHO's 2006 guidelines, which recommend starting treatment at less than 200 cells/mm3. (See Universal access to AIDS treatment for more information). Some countries may have treatment guidelines which differ from WHO recommendations. For example, although USA treatment guidelines state that treatment should be initiated in all patients with a CD4 count <350 cells/mm3 they also recommend treatment for patients with a CD4 count between 350 and 500 cells/mm3. If there are complications, such as if the patient has hepatitis B, an AIDS-defining illness or is pregnant, guidelines usually recommend that treatment is started earlier. WHO clinical staging In poorer countries, CD4 testing may be unavailable due to the expense of the equipment. In these cases, there is a method of describing the different stages of HIV disease based on clinical symptoms, known as the WHO staging system for HIV disease. Where a patient is showing signs of stage 1 and 2 they should not start treatment. However, if they are showing signs of WHO clinical stages 3 or 4 they should start treatment. Clinical stages 3 and 4 are identified by the emergence of certain opportunistic infections (such as PCP) and cancers, which a healthy immune system would normally fight off. Basic clinical assessment Before a person starts treatment, a basic clinical assessment should also be carried out. This assessment determines, for example, existing medical conditions (such as hepatitis, TB, pregnancy, injecting drug use and major psychiatric illness), whether or not the individual is currently taking medications (including traditional and herbal HIV medications), their weight measurement, and a patient's readiness for therapy. Treatment should only be started once the person is ready. A lot of commitment is needed, since following a drug regime can be quite demanding and in most circumstances, the treatment will have to be taken every day for life. Once it is decided that treatment should be started, doctors will give advice about the various HIV drugs and combinations available and which might be most suitable. back to top Choosing the best combination There are a number of issues which need to be considered when choosing a combination of antiretroviral drugs. The first combination of drugs that a person takes is called first-line therapy. In order for HIV treatment to be effective, patients should take a combination of three or four drugs. Antiretroviral drugs attack the ability of HIV to infect healthy cells in five different ways and are therefore divided into five different classes. A typical antiretroviral combination consists of two drugs from the NRTI (nucleoside/nucleotide reverse transcriptase inhibitor) class and one drug from another class. Transmitted HIV drug resistance If possible, a test should be carried out to make sure that a person doesn’t have a strain of HIV that is already resistant to a certain class of drug. If a person’s strain of HIV is resistant to a class of drug, taking that type of drug may be ineffective or at worse, harmful as it may lead to failure of the treatment to work effectively. This type of drug resistance is known as ‘transmitted drug resistance’ because it has been passed from one person to another. Studies have shown that around 1 in 10 HIV infected people in Europe and America are infected with a type of HIV that is already resistant to at least one class of antiretroviral drug before treatment is started.2 Drug interactions Interactions between certain antiretroviral drugs and other drugs, both pharmaceutical and recreational, can alter the effectiveness of antiretroviral therapy. Interactions may lower the amount of antiretroviral drugs absorbed, allowing low level HIV replication to occur, which may increase the risk of drug resistance and thereby lead to treatment failure. Drug interactions are often a concern amongst older people living with HIV, as there is a higher chance they will be taking other medications for age-related illnesses. ARVs may interact with the following types of drugs: Other antiretrovirals: An ongoing study has found that Invirase (saquinavir) when combined with Norvir (ritonavir) may cause an abnormal heart rhythm by affecting the heart's electrical signals.3 Symptoms can range from lightheadedness to an abnormal heartbeat with the possibility that more severe side effects will develop such as ventricular fibrillation.4 This has been found from preliminary data and a review of these findings are ongoing. Other pharmaceutical drugs: Some other pharmaceutical drugs may cause side effects or decrease the effectiveness of some antiretroviral drugs. For example, it is not recommended that protease inhibitors be taken with drugs such as Cafergot and Migranal, which are used to treat migraine headaches.5 Women living with HIV taking oral contraceptives and/or hormone replacement therapy need to talk to their doctor about possible drug interactions. Herbal and complementary treatments: Garlic capsules, for example, stop saquinavir - a protease inhibitor - from working properly.6 Drugs for treating opportunistic infections: For example the tuberculosis treatment rifabutin should usually not be used with the protease inhibitor saquinavir or the NNRTI delavirdine.7 Recreational drugs: Minimal research has been carried out on the relationship between recreational drugs (such as ecstasy, cocaine and amphetamines) and antiretroviral drugs, as many recreational drugs are illegal. However, as most recreational drugs and antiretroviral drugs are broken down in the liver, they may interact and result in serious clinical consequences. Laboratory experiments and case studies have found that the interaction between some recreational drugs and some antiretrovirals results in increased toxicity which increases the risk of potentially fatal side effects such as respiratory depression. However, this has not been determined for all recreational and antiretroviral drugs. The safest action is not to mix these drugs with antiretroviral drugs at all. HIV infected injecting drug users who are taking opioid substitution therapy (such as methadone or bureprenorphine) may be at increased risk of intensified side effects.8 Another risk is that certain antiretrovirals reduce the concentration of the drug substitution therapy leading to withdrawal symptoms.9 However, the effects vary considerably depending on the opioid substitution agent and the antiretroviral drugs taken.10 11 The University of Liverpool maintains an up-to-date chart of drug interactions. An HIV positive man sitting at home before taking his antiretroviral drugs Number of pills Some combinations - especially those involving a protease inhibitor - require swallowing many pills throughout the day, which some people find hard to do. The size of the pills can also be an issue. One option for reducing the pill burden may be to take a FDC (fixed dose combination), which combines two or more drugs in a single tablet or capsule. Food restrictions There are a few drugs, particularly protease inhibitors, which have to be taken with food to improve absorption rates. If taken on an empty stomach, some drugs can be extremely painful to take. In areas where there is no regular access to food therefore, taking these drugs may be unfeasible. However, some other drugs have to be taken on an empty stomach. Storage requirements Storage can be an issue as some HIV drugs have to be kept below a certain temperature to last long term. The older version of ritonavir, for example, must be refrigerated. back to top Monitoring HIV treatment Once a person starts HIV treatment, it is essential that they adhere to their treatment. The patient will need to be monitored by a doctor to make sure that the treatment is working for them. Adherence The term adherence means taking the drugs exactly as described. This includes taking all of the medication at the right time and exactly as the directions state. It also means ensuring that there will be no interactions with other drugs being taken. Anything below 95 percent adherence has been associated with increases in viral load and drug resistance. Therefore adherence to antiretroviral treatment is extremely important. This means missing no more than one dose a month, if taking antiretroviral drug treatment once a day. Viral load monitoring A blank patient treatment record from India Viral load refers to the amount of HIV in the blood. If the viral load is high, T-helper cells tend to be destroyed more quickly. Therefore, the aim of antiretroviral treatment is to keep the viral load as low as possible. In places where it is available, a viral load test is carried out shortly after antiretroviral treatment is started. If the treatment is working effectively, the viral load will drop to the undetectable level – below 50 copies/ml. Ideally this will happen within 24 weeks of starting treatment, but for some it can take 3 to 6 months. On the other hand, some people never reach undetectable. Viral load tests are then carried out every few months. As some viral load tests can produce slightly different results on the same sample of blood, the results are monitored over a period of time. Structured Treatment Interruptions (STIs) A Structured Treatment Interruption (STI) or 'drug holiday' is when someone stops taking antiretroviral treatment temporarily. UK and American treatment guidelines do not recommend taking planned treatment breaks unless under clinical trial settings. Studies have shown that some types of STI have been associated with an increased risk of HIV disease progression.12 13 Side effects Side effects occur when the drugs affect the body in ways other than those intended. Most of the antiretroviral drugs have known side effects, but this does not mean that everyone who takes the drugs will experience them. Some people only experience mild side effects and find them easily manageable. But for some the side effects occur so strongly that they have to consider alternative drugs. Read more about side effects. Immune Reconstitution Inflammatory Syndrome (IRIS) IRIS is an illness that occurs for a small number of patients soon after treatment is started. It is caused by an excessive response by the recovering immune system to opportunistic infections that were already present, but were previously dormant and not producing symptoms. Although the symptoms of IRIS are often mild, occasionally they can be life threatening. Generally those who have a severely damaged immune system before starting antiretroviral treatment are more at risk of developing IRIS.14 IRIS does not indicate that treatment is failing. Usually the best response to IRIS is to continue treatment; the symptoms normally disappear within a few weeks. In cases involving severe opportunistic infections, such as cryptococcal meningitis or tuberculosis, it may be necessary to stop antiretroviral therapy whilst the infection is treated.15 back to top Switching treatment A change of treatment is needed when the antiretrovirals fail to slow down the replication of the virus in the body. This can occur as a result of drug resistance, poor adherence, poor drug absorption or a weak combination of drugs. Increased viral load or an HIV-related illness are signs of treatment failure. Where viral load testing is available, some doctors recommend changing as soon as the viral load starts to rise, although this could mean running out of treatment options more quickly. Others recommend monitoring the trend of the viral load before making a decision to change. However, this approach may increase the risk of developing resistance to certain drugs, which can limit future treatment options. Where viral load testing is not available, the WHO staging system for HIV disease that determines the stage of HIV infection based on clinical symptoms, may be used instead. Combined with clinical judgement, the following table can guide the decision of whether to switch treatment. Treatment failure criteria WHO Stage I WHO Stage II WHO Stage III WHO Stage IV Clinical (CD4 testing unavailable) Do not switch Do not switch Consider switching Switch CD4 failure (viral load testing unavailable) Do not switch repeat CD4 test in three months Do not switch repeat CD4 test in three months Consider switching Switch CD4 failure and viral load failure Consider switching Consider switching Switch Switch Drug resistance Antiretroviral drugs slow the replication of HIV in the body. However the drugs cannot stop the replication completely, so some HIV is able to survive despite ongoing HIV treatment. When HIV replicates it often makes slight mistakes, so each new generation of HIV differs slightly from the one before. These tiny differences in the structure of HIV are called mutations. Some of the mutations occur in the parts of HIV that are targeted by antiretroviral drugs. So although there is some HIV that continues to be attacked by the drugs, there are other strains of HIV that are less likely to be affected. This HIV is called drug resistant HIV, and it is able to replicate unaffected by the drugs. When someone has drug resistant HIV, the amount of HIV in the blood rises and the risk of the person becoming ill increases. Drug resistance is one of the main reasons why antiretroviral treatment fails. If resistance develops, usually the drug regimen needs to be changed. Cross-resistance Resistance to some ARVs can limit future treatment options. If HIV is resistant to one drug, it will sometimes be resistant to similar drugs in the same group. This is called cross-resistance and it means that some antiretroviral drugs will not work even if they have not been used before. Avoiding and detecting resistance There are certain things that can be done to reduce the risk of developing drug resistant HIV. Ensuring that the drug combination is strong to begin with will lessen the risk of resistance developing. This usually means taking a combination of 3 or 4 drugs. Taking medication exactly as prescribed is a very important part of avoiding resistance. Missing doses or not taking them on time lowers the amount of antiretroviral chemicals in the body, which means the virus is not properly suppressed. The virus is then able to replicate faster, increasing the chance of it becoming resistant. Regular viral load testing is also important as the results can indicate whether a drug resistant strain of HIV is developing. If the drug combination is working, the viral load should be undetectable. An increasing viral load can be a sign of growing drug resistance. Salvage treatment Salvage therapy is the term often used to describe the treatment for those who are resistant to drugs in the three original drug classes. In this situation it may be difficult to find a drug regimen that suppresses the viral load to undetectable. Many people start their salvage therapy with a much higher viral load than when they started previous HIV treatments. This puts more pressure on the new combination to work. Each combination used lessens the chance of maintaining a low viral load because of the possibility of developing resistance to the drugs. The choice of new treatment should always depend on what caused the previous one to fail. The introduction of two additional classes of drugs since 2003 (fusion or entry inhibitors and integrase inhibitors) has meant that there are more alternative combinations for those who were running out of treatment options. back to top HIV transmission and antiretroviral drugs Although antiretroviral drugs suppress HIV they do not eliminate the risk of HIV transmission completely, even when the viral load is undetectable. Antiretroviral treatment cannot make HIV disappear from the blood completely. Read our treatment as prevention page as to find out more about the effect of antiretroviral treatment on reducing the risk of HIV prevention. Unprotected sex between two HIV positive people is not a risk-free activity; there are many different strains of HIV and it is possible to become infected with a different strain more than once, which can complicate treatment. Those taking antiretroviral drugs should take as much care to minimise the risk of HIV transmission as they did before starting the treatment. email print tweet more Where Next? AVERT.org has more about: HIV treatment and care Introduction to antiretroviral treatment Stages of HIV infection Universal access Back to top Sign up to our Newsletter Donate References back to top WHO (2009) 'Rapid advice: Antiretroviral therapy for HIV infection in adults and adolescents' Wittkop Linda et. al, (2011, February) 'Effect of transmitted drug resistance on virological and immunological response to initial combination antiretroviral therapy for HIV (EuroCoord-CHAIN joint project): a European multicohort study' 11(5):363-371 Panel on antiretroviral guidelines for adults and adolescents (2011, 10th January) 'Guidelines for the use of antiretroviral agents in HIV-1-infected adults and adolescents' FDA (2010, 23rd February) 'FDA announces possible safety concern for HIV drug combination' www.hiv-druginteractions.org 'Drug interaction charts'. Piscatelli Steven C, et. al, (2002) 'The effect of garlic supplements on the pharmacokinetics of saquinavir' Clinical Infectious Diseases 34(2):234-8 CDC (2008) 'Managing drug interactions in the treatment of HIV-related tuberculosis'. Accessed 9th July 2008 R. Douglas Bruce, M.D., M.A., (October 2007) 'Key interactions between methadone, buprenorphine and HIV medications' ASHM 'DHHS Guidelines for the use of Antiretroviral Agents in HIV-1-Infected Adults and Adolescents, with Australian Commentary' McCance-Katz EF et. al, (2006, December) 'Interactions between buprenorphine and antiretrovirals. II. The protease inhibitors nelfinavir, lopinavir/ritonavir, and ritonavir' Clinical Infectious Diseases 43 Suppl 4:S235-4 Gruber, Valerie A. (2010) 'Methadone, Buprenorphine, and Street Drug Interactions with Antiretroviral Medications' Curr HIV/AIDS Rep 7(3): 152-160 El-Sadr, W & Neaton, J (2006) 'Episodic CD4-guided use of ART is inferior to continuos therapy: results of the SMART study'. CROI 2006 Abstract #106LB, February 2006 Kaufmann, G.R et al (2011) 'Interruptions of cART limits CD4 T-cell recovery and increases the risk for opportunistic complications and death', AIDS 2011, 25:000-000 Monika Müller BA, et. al, (2010) 'Immune reconstitution inflammatory syndrome in patients starting antiretroviral therapy for HIV infection: a systematic review and meta-analysis' 10(4): 251-261 Aidsmap (2010, May 10) 'Risk of IRIS means that HIV treatment should be delayed for patients taking fluconazole for cryptococcal meningitis' Disclaimer & Privacy Policy back to top www.avert.org is an information resource to be used for educational purposes only. 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Deciding when to start antiretroviral treatment depends on the stage of HIV infection which is determined through clinical tests. Once it is decided that an HIV positive patient should start treatment, a variety of factors must be considered when choosing the right combination of drugs for that person. After a person starts treatment, the effectiveness of their treatment must be monitored so that if necessary, the treatment regimen can be switched.
This page discusses these main issues surrounding starting, monitoring and switching HIV treatment in more detail.
There is no proven ‘right’ time to start antiretroviral drug treatment for HIV and AIDS. When a person is diagnosed with HIV, they will not necessarily need to start treatment immediately.
Starting treatment depends on the stage of HIV infection; most guidelines recommend not starting until the advanced stages of HIV infection because it is an important decision with long-term consequences. The decision also depends on the person; children and pregnant women for example are generally advised to start treatment at an earlier stage compared to other people infected with HIV.
In order to decide whether or not an HIV positive patient should start treatment, clinical tests need to be carried out. These tests determine the stage of HIV infection and the individual patient's readiness for drug treatment, which may depend on a variety of factors such as the patient’s medical history.
Usually, the CD4 test is used to determine when a person should start treatment.
HIV attacks a type of immune system cell called the T-helper cell. The T-helper cell plays an essential part in the immune system by helping to co-ordinate all the other cells to fight illnesses. HIV damages and destroys T-helper cells; as a result, there are fewer cells available to help the immune system. A major reduction in the number of T-helper cells can have a serious effect on the immune system.
A CD4 test measures the number of T-helper cells (in a cubic millimetre of blood) which is known as a CD4 count. Someone who is not infected with HIV normally has between 500 and 1200 cells/mm3. In a person infected with HIV, the CD4 count often declines over a number of years.
HIV drug treatment is generally recommended when the CD4 test shows fewer than 350 cells/mm3. World Health Organization (WHO) 2010 guidelines recommend starting treatment for all patients with CD4 counts of <350 cells/mm3 in all countries.1 Although most resource-limited countries aim to follow these guidelines, a number still observe the WHO's 2006 guidelines, which recommend starting treatment at less than 200 cells/mm3. (See Universal access to AIDS treatment for more information).
Some countries may have treatment guidelines which differ from WHO recommendations. For example, although USA treatment guidelines state that treatment should be initiated in all patients with a CD4 count <350 cells/mm3 they also recommend treatment for patients with a CD4 count between 350 and 500 cells/mm3.
If there are complications, such as if the patient has hepatitis B, an AIDS-defining illness or is pregnant, guidelines usually recommend that treatment is started earlier.
In poorer countries, CD4 testing may be unavailable due to the expense of the equipment. In these cases, there is a method of describing the different stages of HIV disease based on clinical symptoms, known as the WHO staging system for HIV disease.
Where a patient is showing signs of stage 1 and 2 they should not start treatment. However, if they are showing signs of WHO clinical stages 3 or 4 they should start treatment. Clinical stages 3 and 4 are identified by the emergence of certain opportunistic infections (such as PCP) and cancers, which a healthy immune system would normally fight off.
Before a person starts treatment, a basic clinical assessment should also be carried out. This assessment determines, for example, existing medical conditions (such as hepatitis, TB, pregnancy, injecting drug use and major psychiatric illness), whether or not the individual is currently taking medications (including traditional and herbal HIV medications), their weight measurement, and a patient's readiness for therapy. Treatment should only be started once the person is ready. A lot of commitment is needed, since following a drug regime can be quite demanding and in most circumstances, the treatment will have to be taken every day for life.
Once it is decided that treatment should be started, doctors will give advice about the various HIV drugs and combinations available and which might be most suitable.
There are a number of issues which need to be considered when choosing a combination of antiretroviral drugs. The first combination of drugs that a person takes is called first-line therapy.
In order for HIV treatment to be effective, patients should take a combination of three or four drugs. Antiretroviral drugs attack the ability of HIV to infect healthy cells in five different ways and are therefore divided into five different classes. A typical antiretroviral combination consists of two drugs from the NRTI (nucleoside/nucleotide reverse transcriptase inhibitor) class and one drug from another class.
If possible, a test should be carried out to make sure that a person doesn’t have a strain of HIV that is already resistant to a certain class of drug. If a person’s strain of HIV is resistant to a class of drug, taking that type of drug may be ineffective or at worse, harmful as it may lead to failure of the treatment to work effectively. This type of drug resistance is known as ‘transmitted drug resistance’ because it has been passed from one person to another.
Studies have shown that around 1 in 10 HIV infected people in Europe and America are infected with a type of HIV that is already resistant to at least one class of antiretroviral drug before treatment is started.2
Interactions between certain antiretroviral drugs and other drugs, both pharmaceutical and recreational, can alter the effectiveness of antiretroviral therapy. Interactions may lower the amount of antiretroviral drugs absorbed, allowing low level HIV replication to occur, which may increase the risk of drug resistance and thereby lead to treatment failure.
Drug interactions are often a concern amongst older people living with HIV, as there is a higher chance they will be taking other medications for age-related illnesses.
ARVs may interact with the following types of drugs:
Other antiretrovirals: An ongoing study has found that Invirase (saquinavir) when combined with Norvir (ritonavir) may cause an abnormal heart rhythm by affecting the heart's electrical signals.3 Symptoms can range from lightheadedness to an abnormal heartbeat with the possibility that more severe side effects will develop such as ventricular fibrillation.4 This has been found from preliminary data and a review of these findings are ongoing.
Other pharmaceutical drugs: Some other pharmaceutical drugs may cause side effects or decrease the effectiveness of some antiretroviral drugs. For example, it is not recommended that protease inhibitors be taken with drugs such as Cafergot and Migranal, which are used to treat migraine headaches.5 Women living with HIV taking oral contraceptives and/or hormone replacement therapy need to talk to their doctor about possible drug interactions.
Herbal and complementary treatments: Garlic capsules, for example, stop saquinavir - a protease inhibitor - from working properly.6
Drugs for treating opportunistic infections: For example the tuberculosis treatment rifabutin should usually not be used with the protease inhibitor saquinavir or the NNRTI delavirdine.7
Recreational drugs: Minimal research has been carried out on the relationship between recreational drugs (such as ecstasy, cocaine and amphetamines) and antiretroviral drugs, as many recreational drugs are illegal. However, as most recreational drugs and antiretroviral drugs are broken down in the liver, they may interact and result in serious clinical consequences. Laboratory experiments and case studies have found that the interaction between some recreational drugs and some antiretrovirals results in increased toxicity which increases the risk of potentially fatal side effects such as respiratory depression. However, this has not been determined for all recreational and antiretroviral drugs. The safest action is not to mix these drugs with antiretroviral drugs at all.
HIV infected injecting drug users who are taking opioid substitution therapy (such as methadone or bureprenorphine) may be at increased risk of intensified side effects.8 Another risk is that certain antiretrovirals reduce the concentration of the drug substitution therapy leading to withdrawal symptoms.9 However, the effects vary considerably depending on the opioid substitution agent and the antiretroviral drugs taken.10 11
The University of Liverpool maintains an up-to-date chart of drug interactions.
Some combinations - especially those involving a protease inhibitor - require swallowing many pills throughout the day, which some people find hard to do. The size of the pills can also be an issue. One option for reducing the pill burden may be to take a FDC (fixed dose combination), which combines two or more drugs in a single tablet or capsule.
There are a few drugs, particularly protease inhibitors, which have to be taken with food to improve absorption rates. If taken on an empty stomach, some drugs can be extremely painful to take. In areas where there is no regular access to food therefore, taking these drugs may be unfeasible. However, some other drugs have to be taken on an empty stomach.
Storage can be an issue as some HIV drugs have to be kept below a certain temperature to last long term. The older version of ritonavir, for example, must be refrigerated.
Once a person starts HIV treatment, it is essential that they adhere to their treatment. The patient will need to be monitored by a doctor to make sure that the treatment is working for them.
The term adherence means taking the drugs exactly as described. This includes taking all of the medication at the right time and exactly as the directions state. It also means ensuring that there will be no interactions with other drugs being taken.
Anything below 95 percent adherence has been associated with increases in viral load and drug resistance. Therefore adherence to antiretroviral treatment is extremely important. This means missing no more than one dose a month, if taking antiretroviral drug treatment once a day.
Viral load refers to the amount of HIV in the blood. If the viral load is high, T-helper cells tend to be destroyed more quickly. Therefore, the aim of antiretroviral treatment is to keep the viral load as low as possible.
In places where it is available, a viral load test is carried out shortly after antiretroviral treatment is started. If the treatment is working effectively, the viral load will drop to the undetectable level – below 50 copies/ml. Ideally this will happen within 24 weeks of starting treatment, but for some it can take 3 to 6 months. On the other hand, some people never reach undetectable.
Viral load tests are then carried out every few months. As some viral load tests can produce slightly different results on the same sample of blood, the results are monitored over a period of time.
A Structured Treatment Interruption (STI) or 'drug holiday' is when someone stops taking antiretroviral treatment temporarily. UK and American treatment guidelines do not recommend taking planned treatment breaks unless under clinical trial settings. Studies have shown that some types of STI have been associated with an increased risk of HIV disease progression.12 13
Side effects occur when the drugs affect the body in ways other than those intended. Most of the antiretroviral drugs have known side effects, but this does not mean that everyone who takes the drugs will experience them. Some people only experience mild side effects and find them easily manageable. But for some the side effects occur so strongly that they have to consider alternative drugs.
Read more about side effects.
IRIS is an illness that occurs for a small number of patients soon after treatment is started. It is caused by an excessive response by the recovering immune system to opportunistic infections that were already present, but were previously dormant and not producing symptoms. Although the symptoms of IRIS are often mild, occasionally they can be life threatening. Generally those who have a severely damaged immune system before starting antiretroviral treatment are more at risk of developing IRIS.14
IRIS does not indicate that treatment is failing. Usually the best response to IRIS is to continue treatment; the symptoms normally disappear within a few weeks. In cases involving severe opportunistic infections, such as cryptococcal meningitis or tuberculosis, it may be necessary to stop antiretroviral therapy whilst the infection is treated.15
A change of treatment is needed when the antiretrovirals fail to slow down the replication of the virus in the body. This can occur as a result of drug resistance, poor adherence, poor drug absorption or a weak combination of drugs. Increased viral load or an HIV-related illness are signs of treatment failure.
Where viral load testing is available, some doctors recommend changing as soon as the viral load starts to rise, although this could mean running out of treatment options more quickly. Others recommend monitoring the trend of the viral load before making a decision to change. However, this approach may increase the risk of developing resistance to certain drugs, which can limit future treatment options.
Where viral load testing is not available, the WHO staging system for HIV disease that determines the stage of HIV infection based on clinical symptoms, may be used instead.
Combined with clinical judgement, the following table can guide the decision of whether to switch treatment.
Antiretroviral drugs slow the replication of HIV in the body. However the drugs cannot stop the replication completely, so some HIV is able to survive despite ongoing HIV treatment.
When HIV replicates it often makes slight mistakes, so each new generation of HIV differs slightly from the one before. These tiny differences in the structure of HIV are called mutations. Some of the mutations occur in the parts of HIV that are targeted by antiretroviral drugs. So although there is some HIV that continues to be attacked by the drugs, there are other strains of HIV that are less likely to be affected. This HIV is called drug resistant HIV, and it is able to replicate unaffected by the drugs.
When someone has drug resistant HIV, the amount of HIV in the blood rises and the risk of the person becoming ill increases. Drug resistance is one of the main reasons why antiretroviral treatment fails. If resistance develops, usually the drug regimen needs to be changed.
Resistance to some ARVs can limit future treatment options. If HIV is resistant to one drug, it will sometimes be resistant to similar drugs in the same group. This is called cross-resistance and it means that some antiretroviral drugs will not work even if they have not been used before.
There are certain things that can be done to reduce the risk of developing drug resistant HIV.
Salvage therapy is the term often used to describe the treatment for those who are resistant to drugs in the three original drug classes. In this situation it may be difficult to find a drug regimen that suppresses the viral load to undetectable.
Many people start their salvage therapy with a much higher viral load than when they started previous HIV treatments. This puts more pressure on the new combination to work. Each combination used lessens the chance of maintaining a low viral load because of the possibility of developing resistance to the drugs. The choice of new treatment should always depend on what caused the previous one to fail.
The introduction of two additional classes of drugs since 2003 (fusion or entry inhibitors and integrase inhibitors) has meant that there are more alternative combinations for those who were running out of treatment options.
Although antiretroviral drugs suppress HIV they do not eliminate the risk of HIV transmission completely, even when the viral load is undetectable. Antiretroviral treatment cannot make HIV disappear from the blood completely.
Read our treatment as prevention page as to find out more about the effect of antiretroviral treatment on reducing the risk of HIV prevention.
Unprotected sex between two HIV positive people is not a risk-free activity; there are many different strains of HIV and it is possible to become infected with a different strain more than once, which can complicate treatment. Those taking antiretroviral drugs should take as much care to minimise the risk of HIV transmission as they did before starting the treatment.
www.avert.org is an information resource to be used for educational purposes only. The information is not intended to serve as a substitute for professional medical advice and we recommend that all decisions about your treatment or products you wish to use should be discussed thoroughly and frankly with your doctor.
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