原发性中枢神经系统淋巴瘤中MYD88和CDKN2A的分子特征及治疗意义
Molecular Characterization and Therapeutic Implications of MYD88 and CDKN2A in Primary CNS Lymphoma.
作者信息
Taomoto Ryouta, Aoki Mikiko, Enomoto Toshiyuki, Inoue Tooru, Nabeshima Kazuki, Hamasaki Makoto, Abe Hiroshi
机构信息
Department of Neurosurgery, Fukuoka University of Medicine, Fukuoka, Japan.
Department of Pathology, Fukuoka University of Medicine, Fukuoka, Japan.
出版信息
Anticancer Res. 2025 Aug;45(8):3441-3450. doi: 10.21873/anticanres.17705.
BACKGROUND/AIM: MYD88L265P mutation and CDKN2A loss are among the earliest reported aberrations identified during clonal evolution in primary central nervous system lymphoma (PCNSL), suggesting their role as driver gene mutations critical to the tumorigenesis of this disease. There is no consensus on the relationship between these mutations and prognosis. This study analyzed the incidence of MYD88L265P mutation and CDKN2A homozygous deletion (HD) in PCNSL in relation to prognosis, and whether they could be potential therapeutic targets.
MATERIALS AND METHODS
Forty-one patients with intracranially localized diffuse large B-cell lymphomas (DLBCL) with known prognosis were included; MYD88L265P mutation was determined using i-densy, MYD88 protein expression using immunostaining, and CDKN2A HD using fluorescence hybridization (FISH). Overall survival (OS) was calculated using the Kaplan-Meier method.
RESULTS
MYD88L265P mutation was found in 35% (7/20) of patients, with a median OS of 14 and 29 months in the mutation-positive and mutation-negative groups, respectively; this was shorter in the mutation-positive group (= 0.6). Immunostaining was positive in 85% (34/40); median OS was 22 and 28.5 months in the immunostaining-positive and immunostaining-negative groups, respectively; this was shorter in the positive group (=0.4). CDKN2A HD was found in 73% (27/37) of patients, with median OS of 15 and 35 months, in the HD-positive and HD-negative groups, respectively; shorter in the HD -positive group (=0.3). When the MYD88L265P mutation and CDKN2A HD were analyzed together, there was a trend toward shorter survival in the group with both mutations (=0.8).
CONCLUSION
The MYD88L265P mutation was present in 35% of patients, and CDKN2A HD was present in 73%. The MYD88L265 mutation and CDKN2A HD, when considered separately, did not individually demonstrate a clear prognostic correlation; however, prognosis varied notably between patients presenting with both mutations compared to those without. The presence or absence of these mutations may be helpful in future treatment selection when the disease becomes relapsed/refractory after initial therapy.
背景/目的:MYD88L265P突变和CDKN2A缺失是原发性中枢神经系统淋巴瘤(PCNSL)克隆进化过程中最早报道的畸变之一,提示它们作为驱动基因突变在该疾病的肿瘤发生中起关键作用。关于这些突变与预后之间的关系尚无共识。本研究分析了PCNSL中MYD88L265P突变和CDKN2A纯合缺失(HD)的发生率与预后的关系,以及它们是否可能成为潜在的治疗靶点。
材料与方法
纳入41例已知预后的颅内局限性弥漫性大B细胞淋巴瘤(DLBCL)患者;使用i-densy检测MYD88L265P突变,免疫染色检测MYD88蛋白表达,荧光杂交(FISH)检测CDKN2A HD。采用Kaplan-Meier法计算总生存期(OS)。
结果
35%(7/20)的患者检测到MYD88L265P突变,突变阳性组和突变阴性组的中位OS分别为14个月和29个月;突变阳性组的OS较短(P=0.6)。免疫染色阳性率为85%(34/40);免疫染色阳性组和免疫染色阴性组的中位OS分别为22个月和28.5个月;阳性组的OS较短(P=0.4)。73%(27/37)的患者检测到CDKN2A HD,HD阳性组和HD阴性组的中位OS分别为15个月和35个月;HD阳性组的OS较短(P=0.3)。当同时分析MYD88L265P突变和CDKN2A HD时,两种突变均有的组生存有缩短趋势(P=0.8)。
结论
35%的患者存在MYD88L265P突变,73%的患者存在CDKN2A HD。单独考虑时,MYD88L265突变和CDKN2A HD均未显示出明确的预后相关性;然而,与无这两种突变的患者相比,同时存在这两种突变的患者预后差异显著。当疾病在初始治疗后复发/难治时,这些突变的有无可能有助于未来的治疗选择。
Zotero 插件