Which statement best describes the relationship between immunoassay screening cutoffs and GC-MS confirmation cutoffs?

Study for the MTLAWS Drug Testing Screening Laboratory Test. Master with flashcards and multiple choice questions and get ready for your exam with detailed explanations and hints.

Multiple Choice

Which statement best describes the relationship between immunoassay screening cutoffs and GC-MS confirmation cutoffs?

Explanation:
Immunoassay screening thresholds are set to flag potential positives based on assay performance, including sensitivity, specificity, and how much cross-reactivity can occur with similar compounds. Because these screens trade off false positives against false negatives, the cutoff can end up higher or lower depending on how the lab balances the risk of missing a true case versus burdening confirmatory testing with false alarms. GC-MS confirmation, on the other hand, identifies a specific analyte by its mass spectrum and retention time, using definitive, instrument-specific criteria. You look for particular fragment ions, exact retention times, and consistent spectral patterns, which makes the method highly specific and typically more sensitive at the detection limit than a screening test. Putting that together, the screening cutoff may be higher or lower than the GC-MS confirmation cutoff depending on the test and analyte, and GC-MS relies on its precise, instrument-driven criteria with often lower detection limits and explicit retention time/fragment ion requirements. This two-tier setup—broad initial screening followed by precise confirmation—helps ensure both broad detection and reliable identity.

Immunoassay screening thresholds are set to flag potential positives based on assay performance, including sensitivity, specificity, and how much cross-reactivity can occur with similar compounds. Because these screens trade off false positives against false negatives, the cutoff can end up higher or lower depending on how the lab balances the risk of missing a true case versus burdening confirmatory testing with false alarms.

GC-MS confirmation, on the other hand, identifies a specific analyte by its mass spectrum and retention time, using definitive, instrument-specific criteria. You look for particular fragment ions, exact retention times, and consistent spectral patterns, which makes the method highly specific and typically more sensitive at the detection limit than a screening test.

Putting that together, the screening cutoff may be higher or lower than the GC-MS confirmation cutoff depending on the test and analyte, and GC-MS relies on its precise, instrument-driven criteria with often lower detection limits and explicit retention time/fragment ion requirements. This two-tier setup—broad initial screening followed by precise confirmation—helps ensure both broad detection and reliable identity.

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