ATC kod: L01CD02
En del studier visar att kvinnligt kön är korrelerat med högre risk för biverkningar av docetaxel. Data om könsrelaterade skillnader i farmakokinetik (PK) för docetaxel är kontroversiella men en del studier visar på något högre exponering hos kvinnor.
Generally, women mount stronger innate and adaptive immune responses than men [1]. Women with lung cancer have a more favorable survival compared to men [2]. The 5-year survival is 17 percent among men, and 24 percent among women, in Sweden [3].
The incidence of lung cancer has decreased among men since from 1980s but has increased significantly among women, which reflects women's changing smoking habits. Now the proportion of smoking women is greater than the proportion of smoking men. In Sweden lung cancer made up 6.1% of all yearly cases of cancer, year 2016. The incidence was higher among women (6.8%, n=2067), compared to men (5.4% , n=1824) [3]
Due to the product information there is no sex-related difference in docetaxel PK, and no sex differentiation in dosing has been suggested [4]. However, there are some data indicating sex differences in PK of docetaxel. A study found that women had a 35% lower docetaxel clearance than men (51 men, 41 women) and a gender effect on docetaxel metabolism was suggested [5]. While other studies found no clear effect of patient’s sex on docetaxel PK [6, 7].
Lower AUC has been observed in premenopausal women [8], and also castrated men showed increased docetaxel clearance and a 2-fold decrease in AUC [9]. Therefore a review article suggests that hormonal factors such as castration status and menopausal status could be part of the underlying mechanisms explaining the discrepancy in the influence of patient's sex on docetaxel pharmacokinetics [10].
Docetaxel binds strongly to serum alpha1-acid glycoprotein and concentration of this protein is lower in young women compared to men and women in higher ages, and due to the fact that the expression and activity of CYP3A4, the main docetaxel metabolizing enzyme, is higher in women. Therefore authors of the “Sex and Dender Differences in Pharmacology” book hypothesis that with standard dosing, the concentration of free drug might be much higher in young- and middle-aged women compared to men [2]. Women on average display higher expression and activity of CYP3A4. Sex-related differences in exposure could be of relevance for several substrates of the CYP3A family [2].
There are no published data indicating sex-related difference in docetaxel efficacy. Considering the probability of higher exposure to docetaxel in women, especially in younger ages, and reports on increased risk of side effects among women, sex-related difference in efficacy is a probability that has not been studied.
Due to European Medicines Agency, the onset of nausea, headache, skin local toxicity, and rash/itch have been seen more frequently in women (62 TCF (docetaxel/cisplatin/5-fluorouracil)-treated subjects) than in men (159 TCF-treated subjects) [11].
A population PK-PD model included 637 patients (272 men, 365 women) with carcinoma, melanoma, and sarcoma who had been enrolled in 24 open uncontrolled trials. The model indicated that female patients treated with docetaxel are at increased risk for severe neutropenia [12].
Docetaxel, like other mitosis inhibitors, may be harmful to the fetus and should not be given during early pregnancy. For more information regarding teratogenic aspects, please consult Janusmed Drugs and Birth Defects (in Swedish, Janusmed fosterpåverkan).
Läkemedel innehållande docetaxel (ATC-kod L01CD02 ) används huvudsakligen på sjukhus och därför saknas könsspecifika användningsdata [13].
Uppdaterat: 2021-01-01
Litteratursökningsdatum: 2020-10-01
Faktagranskat av: Diana Rydberg, Carl-Olav Stiller
Godkänt av: Karin Schenck-Gustafsson