The Effects of Cumulative Dose and Polymorphisms in CYP2B6 on the Mitotane Plasma Trough Concentrations in Chinese Patients With Advanced Adrenocortical Carcinoma

Liu, Xin; Shang, Junmei; Fu, Qiang; Li, Lin; Deng, Jianhua; Tang, Yan; Li, Jiantao; Mei, Dan; Zhang, Bo; Zhang, Shuyang

doi:10.3389/fonc.2022.919027

Cited by 1 publication

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“…The polymorphism of CYP enzymes could be involved in the individual variability of the therapeutic effect of mitotane. It has been demonstrated that CYP2B6 is a key cytochrome for mitotane metabolism and that its genetic profile can predict the circulating concentration of mitotane ( 28 – 30 ). In fact, patients with the wild-type “G” allele achieved lower mitotane concentrations than the patient carrying the mutant “T” allele ( 28 ).…”

Section: Discussionmentioning

confidence: 99%

Neurological adverse events of mitotane in adrenocortical carcinoma: results of a pilot study

Mormando,

Galiè,

Bianchini

et al. 2023

Front. Oncol.

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IntroductionMitotane, the only drug approved by the Food and Drug Administration (FDA) for the treatment of adrenocortical carcinoma, is associated with several side effects including neurotoxicity. The aim of our study is to investigate the relationship between mitotane plasma levels and neurological toxicity.MethodsWe have considered five patients affected by adrenocortical carcinoma treated with mitotane. The neurological assessment included a neurological examination, an electroencephalogram, event-related potentials (P300), and a neuropsychological assessment. All of the patients were first considered at the onset of symptoms of neurotoxicity or when mitotanemia levels were above 18 mg/L, for the second time at mitotanemia normalization and subsequently at its further increase, or in case of persistent neurological abnormalities, some months after normalization.ResultsAt the first neurotoxicity, four patients showed impaired neurological examination, electroencephalogram, and P300; three patients had impaired neuropsychological assessment; one patient, only P300. At mitotanemia normalization, the neurological examination became normal in all patients and electroencephalogram normalized in one patient, improved in another one, continuing to be altered in the other three. P300 latency and neuropsychological assessment normalized in two patients and persisted altered in the patient experiencing long-term mitotane toxicity. At the third evaluation, in the patient with prolonged mitotane toxicity, the normal mitotanemia in the previous 9 months restored P300 and improved the electroencephalogram but not the neuropsychological assessment. In the two patients experiencing a further rise of mitotanemia, neurological examination was normal but P300 and electroencephalogram were altered.ConclusionThe results of our study highlighted the presence of neurophysiological and neuropsychological abnormalities associated with mitotane values above 18 mg/L.

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Section: Discussionmentioning

confidence: 99%