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HelpTest Code LABHIRGT Human Immunodeficiency Virus 1 Drug Resistance by Next Generation Sequencing
Additional Codes
| Test Name in EPIC | Epic Test Code | Mnemonic | ARUP Test ID |
|---|---|---|---|
| HIV-1 RNA GENO PR-RT RESIST, P |
LABHIRGT |
HIV1 NGS | 3003853 |
Useful For/Utility
Provides antiretroviral susceptibility information for protease inhibitors (PI), reverse transcriptase inhibitors (NRTI, NNRTI), and integrase inhibitors (INT). Intended for patients with viral load >500 copies/mL.
Methodology
Massively Parallel Sequencing
Specimen Requirements
Collect
Lavender (EDTA), pink (K2EDTA), or plasma preparation tube.
Specimen Preparation
Separate plasma from cells within 24 hours. Transfer 3.0 mL plasma to an ARUP standard transport tube. (Min: 2.5 mL)
Storage/Transport Temperature
Frozen.
Unacceptable Conditions
Serum. Heparinized specimens.
Remarks
Please submit most recent viral load and test date, if available.
Stability
After separation from cells: Ambient: 24 hours; Refrigerated: 72 hours; Frozen: 3 months
Specimen Transport Temperature
Ship Frozen
Test Classification and CPT Coding
CPT: 87900; 87901; 87906
LOIN-C
Component Test Code* Component Chart Name LOINC
3003854 HIV-1 Drug Resistance by NGS 80689-3
3003855 EER HIV-1 Drug Resistance by NGS 11502-2
Day(s) Performed
Sunday-Saturday
Reported in 4-10 days
Reference Values
Susceptible or Resistance
Interpretation
This assay predicts HIV-1 resistance to protease inhibitors, nucleoside reverse transcriptase inhibitors, non-nucleoside reverse transcriptase inhibitors, and integrase inhibitors. The protease gene, integrase gene, and the reverse transcriptase gene of the viral genome are sequenced using next generation sequencing. Drug resistance is assigned using the Stanford hivdb database.
This test should be used in conjunction with clinical presentation and other laboratory markers. A patient's response to therapy depends on multiple factors, including patient adherence, percentage of resistant virus population, dosing, and drug pharmacology issues.
This test detects populations down to 10 percent of the total population which may account for resistance interpretation differences between methods. Some insertions or deletions may be difficult to detect using this software.
Drug Resistance Interpretations are defined as follows:
-Not Determined indicates incomplete sequence coverage across a given gene or genes.
-Susceptible indicates no drug resistance mutations (DRMs) were detected.
-Potential Low-Level Resistance indicates the presence of DRMs that suggest prior antiretroviral (ARV) exposure or are associated with resistance only when they occur alongside other DRMs.
-Low-Level Resistance indicates the presence of DRMs that are associated with reduced in vitro ARV susceptibility or a suboptimal virological response to ARV treatment.
-Intermediate Resistance indicates that while there is a high likelihood of reduced ARV activity due to the virus's DRMs, the ARV is still expected to retain significant antiviral activity.
-High-Level Resistance indicates the presence of DRMs predicted to confer a level of resistance similar to that seen in viruses with the highest levels of reduced in vitro susceptibility or those with little to no virological response to ARV treatment.
Mutations are classified as follows:
-Drug Resistance Mutations reduce susceptibility of specific drug classes whether found in isolation or in combination with other drugs.
-Accessory Mutations reduce susceptibility of specific drug classes only when found in combination with drug resistance mutations.
-Additional mutations have cleared or approved by the US Food and Drug Administration associated with drug resistance.
-Uncalled mutation sites are known locations of drug resistance mutations that have an inadequate number of sequencing reads to accurately determine if mutations are present.