不确定性中的确定性:确定血液恶性肿瘤中意义不确定变异的重新分类率和原因

EJHaem Pub Date : 2024-09-12 DOI:10.1002/jha2.1002
Anoop K. Enjeti, Natasha Walker, Oliver Fahey, Elizabeth Johnston, Hannah Legge-Wilkinson, Nateika Ramsurrun, Jonathan Sillar, Lisa F. Lincz, Andrew Ziolkowski, David Mossman
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引用次数: 0

摘要

导言:随着大规模平行测序诊断技术的广泛应用,意义不确定的变异(VUS)在癌症中被普遍报道。血液恶性肿瘤患者的 VUS 重新分类率尚无定论,我们对此进行了回顾性评估。我们还调查了在初始分类后 12-24 个月或超过 24 个月重新评估 VUS 是否有意义。 方法 对2018年9月至2021年12月期间转诊至澳大利亚纽卡斯尔约翰-亨特医院分子医学科的血液恶性肿瘤患者进行回顾性审计。对数据进行了VUS分析,然后使用现行体细胞变异指南在标准软件中进行了重新分析。基线时的 VUS 比例与重新分析后的比例进行了比较。 结果 患者队列(n = 944)中最常见的诊断是急性髓性白血病(41%)、骨髓增生异常综合征(31%)和慢性粒细胞白血病(7%)。共对 210 例 VUS 进行了重新分析。最常见的 VUS 位于 TET2(20%)、RUNX1(10%)和 DNMT3A(9%)基因中。共有 103 个变异在初次分类后 24 至 39 个月内进行了重新分析,107 个变异在初次分类后 12 至 24 个月内进行了重新分析。其中,33 个(16%)VUS 在初始分类后 24-39 个月时被重新分类,12 个(11%)在初始分类后 12-24 个月时被重新分类。两组中最常见的重新分类变异为 CSF3R(32%)、TET2(29%)、ASXL1(11%)和 ZRSR2(11%)。 结论 这项关于血癌 VUS 重新分类的研究表明,每 7 例 VUS 中就有 1 例在初始分类后 12 个月被重新分类。这可以为实践指南提供参考,并对血液恶性肿瘤的预后、诊断和治疗产生潜在影响。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Certainty in uncertainty: Determining the rate and reasons for reclassification of variants of uncertain significance in haematological malignancies

Certainty in uncertainty: Determining the rate and reasons for reclassification of variants of uncertain significance in haematological malignancies

Introduction

Variants of uncertain significance (VUS) are commonly reported in cancer with the widespread adoption of diagnostic massive parallel sequencing. The rate of reclassification of VUS in patients with haematological malignancy is not known and we evaluated this retrospectively. We also investigated whether re-evaluating VUS in 12–24 months or greater than 24 months post-initial classification was significant.

Method

A retrospective audit of patients with haematological malignancies referred to the Molecular Medicine Department at the John Hunter Hospital in Newcastle, Australia between September 2018 and December 2021. Data was analysed for VUS, which was then re-analysed in standard software using current somatic variant guidelines. Proportions of VUS at baseline were compared to post-re-analysis.

Results

The most common diagnoses in the patient cohort (n = 944) were acute myelogenous leukaemia (41%), myelodysplastic syndrome (31%), and chronic myelomonocytic leukaemia (7%). A total of 210 VUS were re-analysed. The most common VUS were in the TET2 (20%), RUNX1 (10%) and DNMT3A (9%) genes. A total of 103 were re-analysed at 24–39 months post-initial classification and 107 variants were re-analysed between 12 and 24 months post-initial classification. Of these, 33 (16%) of VUS were re-classified at 24–39 months and 12 (11%) were re-classified at 12–24 months post-initial classification. The most common variants that were re-classified in both groups were CSF3R (32%), TET2 (29%), ASXL1 (11%) and ZRSR2 (11%).

Conclusion

This study on reclassification of VUS in blood cancers demonstrated that one in seven VUS were re-classified 12 months post initial classification. This can inform practice guidelines and potentially impact the prognosis, diagnosis and treatment of haematological malignancies.

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