Factors Compromising Glucuronidase Performance in Urine Drug Testing Potentially Resulting in False Negatives

Next generation beta-glucuronidases can effectively cleave glucuronides in urine at room temperature. However, during the discovery studies, additional challenges were identified for urine drug testing across biologically relevant pH extremes and patient urine specimens. Different enzymes were evaluated across clinical urine specimens and commercially available urine control matrices. Each enzyme shows distinct substrate preferences, pH optima, and variability across clinical specimens. These results demonstrate how reliance on a single glucuronidated substrate as the internal hydrolysis control cannot ensure performance across a broader panel of analytes. Moreover, sample specific urine properties compromise beta-glucuronidases to varying levels, more pronounced for some enzymes, and thereby lower the recovery of some drug analytes in an enzyme-specific manner. A minimum of 3-fold dilution of urine with buffer yields measurable improvements in achieving target pH and reducing the impact of endogenous compounds on enzyme performance. After subjecting the enzymes to pH extremes and compromising chemicals, one particular beta-glucuronidase was identified that addressed many of these challenges and greatly lower the risk of failed hydrolyses. In summary, we present strategies to evaluate glucuronidases that aid in higher accuracy urine drug tests with lower potential for false negatives.

Automated summary

Different enzymes exhibit varying performances in clinical urine specimens, showing distinct substrate preferences and pH optima. Urine-specific properties affect the hydrolytic effectiveness of beta-glucuronidases, with some enzymes being more significantly impacted. Diluting urine with buffer greatly improves achieving target pH and reduces the impact of endogenous compounds on enzyme performance.