Literature DB >> 19179423

Risk analysis of severe myelotoxicity with temozolomide: the effects of clinical and genetic factors.

Terri S Armstrong1, Yumei Cao, Michael E Scheurer, Elizabeth Vera-Bolaños, Rochelle Manning, Mehmet F Okcu, Melissa Bondy, Renke Zhou, Mark R Gilbert.   

Abstract

A benefit of temozolomide (TMZ) is that myelotoxicity is uncommon. Recently, several small series have reported significant myelotoxicity resulting in treatment delays or death. The ability to predict risk of myelotoxicity may influence patient care. We retrospectively reviewed 680 malignant glioma patients and developed a clinical risk formula for myelotoxicity for each gender by logistic regression. The variables that remained were assigned a score of 1 and added together for a final risk score. Women experienced more myelotoxicity than did men (p = 0.015). For males, risk factors included body surface area (BSA) > or = 2 m(2) (odds ratio [OR] = 2.712, p = 0.04), not on steroids (OR = 2.214, p = 0.06), and on bowel medication (OR = 3.955, p = 0.008). For females, final factors included no prior chemotherapy (OR = 3.727, p = 0.001), creatinine > or = 1 mg/dl (OR = 6.08, p = 0.002), platelets < 270,000/mm(3) (OR = 2.438, p = 0.03), BSA < 2 m(2) (OR = 4.178, p = 0.04), not on medication for gastroesophageal reflux disease (OR = 2.942, p = 0.01), and on analgesics (OR = 2.169, p = 0.05). Age was included because of observable trends. Risk of developing myelotoxicity ranged from 0% to 33% (male) and from 0% to 100% (females). Polymorphisms in NQO1 (NAD(P)H dehydrogenase, quinone 1), MGMT (O(6)-methylguanine-DNA methyltransferase), and GSTP1 (glutathione S-transferase pi 1) were related to risk of developing myelotoxicity in a subset of patients. Myelotoxicity with TMZ is a significant clinical issue for those at risk. Use of a clinical model to predict risk and evaluation of identified genetic polymorphisms related to myelotoxicity may allow for individualized dosing, optimizing patient management.

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Year:  2009        PMID: 19179423      PMCID: PMC2802402          DOI: 10.1215/15228517-2008-120

Source DB:  PubMed          Journal:  Neuro Oncol        ISSN: 1522-8517            Impact factor:   12.300


  19 in total

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Review 9.  Gender differences in pharmacological response.

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  24 in total

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Journal:  J Neurooncol       Date:  2012-03-10       Impact factor: 4.130

Review 2.  Patient profiling for treatment toxicity: potential use of clinical and genomic factors.

Authors:  Terri S Armstrong; Mark R Gilbert
Journal:  Curr Oncol Rep       Date:  2011-02       Impact factor: 5.075

3.  Impact of concurrent versus adjuvant chemotherapy on the severity and duration of lymphopenia in glioma patients treated with radiation therapy.

Authors:  Alexander J Lin; Jian L Campian; Caressa Hui; Soumon Rudra; Yuan J Rao; Dinesh Thotala; Dennis Hallahan; Jiayi Huang
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Review 4.  The FDA NIH Biomarkers, EndpointS, and other Tools (BEST) resource in neuro-oncology.

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8.  Glutathione S-transferase P1 single nucleotide polymorphism predicts permanent ototoxicity in children with medulloblastoma.

Authors:  Surya Rednam; Michael E Scheurer; Adekunle Adesina; Ching C Lau; Mehmet Fatih Okcu
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9.  Persistent bone marrow depression following short-term treatment with temozolomide.

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Authors:  Frank Saran; Olivier L Chinot; Roger Henriksson; Warren Mason; Wolfgang Wick; Timothy Cloughesy; Sunita Dhar; Emanuela Pozzi; Josep Garcia; Ryo Nishikawa
Journal:  Neuro Oncol       Date:  2016-01-24       Impact factor: 12.300

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