INTRODUCTION
The domain covers competencies that are required to initiate therapy and apply protocol adherence measures. A concept adopted by NDoH which advocates that 90% of people who know their HIV status will receive treatment with at least 90% of those on treatment being virally suppressed.
The competencies required in the domain for testing and diagnosis of HIV are:
| 2.1 |
Demonstrate knowledge of ART Principles; |
| 2.2 |
Prepare patients for ART adherence; |
| 2.3 |
Identify, classify, and analyse the various types of ARTs and their side effects and toxicities; |
| 2.5 |
Analyse ART medicine choices in PrEP and PEP, and considerations around pharmacology and drug interactions, including TPT; |
| 2.6 |
Identify and manage PrEP, PEP and ART contra-indications; and |
| 2.7 |
Conduct PEP in the PIMART environment. |
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DOMAIN 2: INITIATE PRE-EXPOSURE PROPHYLAXIS (PrEP), POST-EXPOSURE PROPHYLAXIS (PEP) AND 1ST LINE ANTIRETROVIRAL THERAPY (ART) PLUS INITIATION OF TB-PREVENTATIVE THERAPY (TPT) WHERE APPROPRIATE AND APPLY PROTOCOL ADHERENCE MEASURES
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COMPETENCIES
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BEHAVIOURAL STATEMENTS
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| 2.1 |
Demonstrate knowledge of ART Principles |
|
| 2.1.1 |
Describing the objectives of ART. |
| 2.1.2 |
Describing the HIV life cycle, CD 4 counts, viral load and when to start therapy. |
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| 2.2 |
Prepare patients for ART adherence |
|
| 2.2.1 |
Defining ART adherence. |
| 2.2.2 |
Applying the pre-ART counselling process. |
| 2.2.3 |
Prepare patients for ART by applying the adherence counselling process. |
| 2.2.4 |
Interpreting viral load results and monitor for ART adherence. |
| 2.2.5 |
Conducting laboratory monitoring for antiretroviral therapy efficacy and safety. |
| 2.2.6 |
Applying the post-ART counselling process. |
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| 2.3 |
Identify, classify, and analyse the various types of ART and their side effects and toxicities |
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| 2.3.1 |
Demonstrating knowledge of the classes of ART. |
| 2.3.2 |
Describing the pharmacology, dosing, side effects, toxicity monitoring and management of medicines used in 1st line ART, PrEP and PEP according to current national guidelines. |
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| 2.4.1 |
Describing first-line treatment pharmacology practicalities in PIMART. |
| 2.4.2 |
Identifying who is not eligible for therapy via PIMART by analysing initiation limitations in PIMART. |
Range: TB, IRIS, cryptococcal meningitis, hepatitis B, pregnant woman, patients under 15 years.
| 2.4.3 |
Describing ART Initiation steps and implementing the ART initiation algorithm according to current national guidelines. |
| 2.4.4 |
Transitioning a patient from PrEP to ART if required. |
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| 2.5 |
Analyse ART medicine choices in PrEP and PEP, and considerations around pharmacology and drug interactions, including TPT |
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| 2.5.1 |
Describing and analysing pharmacology, dosing, toxicity, side effects and drug interactions of various regimens as determined by NDoH for PEP and PrEP. |
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| 2.6 |
Identify and manage PrEP, PEP and ART contraindications |
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| 2.6.1 |
Identifying PEP contraindications. |
| 2.6.2 |
Analysing and classifying the management of ambiguities in source status, source ART adherence, and patient HIV status. |
| 2.6.3 |
Referring pregnant and breastfeeding women who require PEP. |
| 2.6.4 |
Describing Hepatitis B screening and vaccination as set out in the PHC EML for PEP. |
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| 2.7 |
Conduct PEP in the PIMART environment |
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| 2.7.1 |
Describing PEP in the PIMART Context. |
| 2.7.2 |
Listing PEP Indications. |
| 2.7.3 |
Identifying at-risk groups in terms of PEP. |
| 2.7.4 |
Analysing PEP Efficacy. |
| 2.7.5 |
Describing the steps in the PEP treatment process. |
| 2.7.6 |
Initiate clients on PEP. |
| 2.7.7 |
Implementing adherence monitoring and follow-up. |
| 2.7.8 |
Implementing the PEP to PrEP transition. |
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Statistics Act, 1999
