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  • Cyclophosphamide exposure assessed with the biomarker phosphoramide mustard-hemoglobin in breast cancer patients: The TailorDose I study.

Cyclophosphamide exposure assessed with the biomarker phosphoramide mustard-hemoglobin in breast cancer patients: The TailorDose I study.

Scientific reports (2021-02-03)
S A M Gernaat, H von Stedingk, M Hassan, H P Nilsson, K A Rodriguez-Wallberg, E Hedayati, P Rydberg
ABSTRACT

Cyclophosphamide (CPA) dosing by body surface area (BSA, m2) has been questioned as a predictor for individual drug exposure. This study investigated phosphoramide mustard-hemoglobin (PAM-Hb, pmol g-1 Hb) as a biomarker of CPA exposure in 135 female breast cancer patients receiving CPA during three courses based on BSA: 500Ā mg/m2 (C500 group, nā€‰=ā€‰67) or 600Ā mg/m2 (C600 group, nā€‰=ā€‰68). The inter-individual difference was calculated for both groups by dividing the highest through the lowest PAM-Hb value of each course. The inter-occasion difference was calculated in percentage for each individual by dividing their PAM-Hb value through the group mean per course, and subsequently dividing this ratio of the latter through the previous course. A multivariable linear regression (MLR) was performed to identify factors that explained the variation of PAM-Hb. During the three courses, the inter-individual difference changed from 3.5 to 2.1 and the inter-occasion difference ranged between 13.3% and 11.9% in the C500 group. In the C600 group, the inter-individual difference changed from 2.7 to 2.9 and theĀ inter-occasion difference ranged between 14.1% and 11.7%. The MLR including BSA, age, GFR, and albumin explained 17.1% of the variation of PAM-HbĀ and was significantly better then the model including only BSA. These factors should be considered when calculating the first dose of CPA for breast cancer patients.

MATERIALS
Product Number
Brand
Product Description

Sigma-Aldrich
Phosphoramide mustard cyclohexylamine, ≥95% (HPLC)