Department of Internal Medicine I (Oncology, Hematology, Clinical Immunology, and Rheumatology), Saarland University Medical Center, Homburg/Saar, Germany.
Institute for Medical Informatics, Statistics and Epidemiology, Leipzig University, Leipzig, Germany.
Ann Hematol. 2024 Nov;103(11):4599-4606. doi: 10.1007/s00277-024-05973-9. Epub 2024 Sep 4.
Vincristine-induced peripheral neuropathy (VIPN) is an adverse effect of regimens used for the treatment of aggressive B-cell non-Hodgkin lymphoma (B-NHL). A single-nucleotide polymorphism (SNP) in the promotor region of the CEP72 gene has been identified as risk factor for the development of VIPN in children. To validate these results in adults we aimed to determine the association of the high-risk CEP72 (rs924607 TT genotype) with the occurrence and severity of VIPN. Analysis of SNP rs924607 (TT, CC or CT) was performed in all enrolled patients with available blood samples with a TaqMan genotyping assay. Rates and grades of VIPN were assessed prospectively as part of the RICOVER-60 trial. CEP72 genotype could be assessed in 519 patients. VIPN data was available for 499/519 patients who were included in the final analysis. 286 (57%) patients developed VIPN of any grade during treatment. Grade 2-4 VIPN occurred in 33% (166/499) of patients. The high-risk CEP72 TT genotype at rs924607 was identified in 97/499 (19%) patients. The TT genotype was not correlated with VIPN in the overall study population compared to patients with either CC or CT genotypes (p = 0.748). However, in the subgroup of female patients, the TT genotype was associated with increased occurrence of any-grade VIPN as well as grade 2-4 VIPN as compared to patients with either CC or CT genotypes (p = 0.016 and p = 0.020, respectively). Thus, the SNP rs924607 in the CEP72 gene is associated with increased VIPN incidence in female patients with aggressive B-NHL treated with CHOP chemotherapy. Trial registration ClinicalTrials.gov identifier: NCT00052936, submission date: 2005-06-23, EudraCT Number: 2010-019587-36.
长春新碱诱导的周围神经病(VIPN)是用于治疗侵袭性 B 细胞非霍奇金淋巴瘤(B-NHL)的方案的一种不良反应。CEP72 基因启动子区域的单核苷酸多态性(SNP)已被确定为儿童 VIPN 发展的危险因素。为了在成人中验证这些结果,我们旨在确定高危 CEP72(rs924607 TT 基因型)与 VIPN 的发生和严重程度的关联。在所有有可用血液样本的入组患者中,使用 TaqMan 基因分型检测分析 SNP rs924607(TT、CC 或 CT)。作为 RICOVER-60 试验的一部分,前瞻性评估 VIPN 的发生率和严重程度。可以评估 519 名患者的 CEP72 基因型。VIPN 数据可用于 499/519 名纳入最终分析的患者。286 名(57%)患者在治疗期间发生任何等级的 VIPN。33%(166/499)的患者发生 2-4 级 VIPN。在 499 名患者中,有 97 名(19%)患者发现 rs924607 处的高危 CEP72 TT 基因型。与 CC 或 CT 基因型的患者相比,TT 基因型在整个研究人群中与 VIPN 无关(p=0.748)。然而,在女性患者亚组中,与 CC 或 CT 基因型的患者相比,TT 基因型与任何等级 VIPN 以及 2-4 级 VIPN 的发生增加相关(p=0.016 和 p=0.020)。因此,CEP72 基因中的 SNP rs924607 与接受 CHOP 化疗的侵袭性 B-NHL 女性患者 VIPN 发生率增加相关。
试验注册
ClinicalTrials.gov 标识符:NCT00052936,提交日期:2005-06-23,EudraCT 编号:2010-019587-36。
