Youngeun Lee, Soo Hyun Seo, Jinho Kim, Sang-A Kim, Ji Yun Lee, Jeong-Ok Lee, Soo-Mee Bang, Kyoung Un Park, Sang Mee Hwang
{"title":"基于单个三级中心经验的 JAK2-未突变红细胞增多症诊断调查方法","authors":"Youngeun Lee, Soo Hyun Seo, Jinho Kim, Sang-A Kim, Ji Yun Lee, Jeong-Ok Lee, Soo-Mee Bang, Kyoung Un Park, Sang Mee Hwang","doi":"10.1007/s40291-024-00703-3","DOIUrl":null,"url":null,"abstract":"<h3 data-test=\"abstract-sub-heading\">Introduction</h3><p>Erythrocytosis is attributed to various clinical and molecular factors. Many cases of <i>JAK2</i>-unmutated erythrocytosis remain undiagnosed. We investigated the characteristics and causes of <i>JAK2</i>-unmutated erythrocytosis.</p><h3 data-test=\"abstract-sub-heading\">Methods</h3><p>We assessed the clinical and laboratory results of patients with erythrocytosis without <i>JAK2</i> mutations and performed targeted next-generation sequencing (NGS) panels for somatic and germline mutations.</p><h3 data-test=\"abstract-sub-heading\">Results</h3><p>In total, 117 patients with <i>JAK2</i>-unmutated erythrocytosis were included. The median hemoglobin and hematocrit levels were 17.9 g/dL and 53.4%, respectively. Erythropoietin levels were not below the reference range. Thrombotic events were reported in 17 patients (14.5%). Among <i>JAK2</i>-unmutated patients, 44 had undergone targeted panel sequencing consisting of myeloid neoplasm-related genes, and 16 had one or more reportable variants in <i>ASXL1</i> (5/44), <i>TET2</i>, <i>CALR</i>, <i>FLT3</i>, and <i>SH2B3</i> (2/44). Additional testing for germline causes revealed eight variants in seven genes in eight patients, including <i>NF1</i>, <i>BPGM</i>, <i>EPAS1</i>, <i>PIEZO1</i>, <i>RHAG</i>, <i>SH2B3</i>, and <i>VHL</i> genes. One <i>NF1</i> pathogenic, one <i>BPGM</i> likely pathogenic, and six variants of undetermined significance were detected.</p><h3 data-test=\"abstract-sub-heading\">Conclusion</h3><p>Somatic and germline mutations were identified in 36.4% and 33.3 % of the <i>JAK2</i>-unmutated group; most variants had unknown clinical significance. Not all genetic causes have been identified; comprehensive diagnostic approaches are crucial for identifying the cause of erythrocytosis.</p>","PeriodicalId":49797,"journal":{"name":"Molecular Diagnosis & Therapy","volume":"1 1","pages":""},"PeriodicalIF":4.1000,"publicationDate":"2024-04-03","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"","citationCount":"0","resultStr":"{\"title\":\"Diagnostic Approaches to Investigate JAK2-Unmutated Erythrocytosis Based on a Single Tertiary Center Experience\",\"authors\":\"Youngeun Lee, Soo Hyun Seo, Jinho Kim, Sang-A Kim, Ji Yun Lee, Jeong-Ok Lee, Soo-Mee Bang, Kyoung Un Park, Sang Mee Hwang\",\"doi\":\"10.1007/s40291-024-00703-3\",\"DOIUrl\":null,\"url\":null,\"abstract\":\"<h3 data-test=\\\"abstract-sub-heading\\\">Introduction</h3><p>Erythrocytosis is attributed to various clinical and molecular factors. Many cases of <i>JAK2</i>-unmutated erythrocytosis remain undiagnosed. We investigated the characteristics and causes of <i>JAK2</i>-unmutated erythrocytosis.</p><h3 data-test=\\\"abstract-sub-heading\\\">Methods</h3><p>We assessed the clinical and laboratory results of patients with erythrocytosis without <i>JAK2</i> mutations and performed targeted next-generation sequencing (NGS) panels for somatic and germline mutations.</p><h3 data-test=\\\"abstract-sub-heading\\\">Results</h3><p>In total, 117 patients with <i>JAK2</i>-unmutated erythrocytosis were included. The median hemoglobin and hematocrit levels were 17.9 g/dL and 53.4%, respectively. Erythropoietin levels were not below the reference range. Thrombotic events were reported in 17 patients (14.5%). Among <i>JAK2</i>-unmutated patients, 44 had undergone targeted panel sequencing consisting of myeloid neoplasm-related genes, and 16 had one or more reportable variants in <i>ASXL1</i> (5/44), <i>TET2</i>, <i>CALR</i>, <i>FLT3</i>, and <i>SH2B3</i> (2/44). Additional testing for germline causes revealed eight variants in seven genes in eight patients, including <i>NF1</i>, <i>BPGM</i>, <i>EPAS1</i>, <i>PIEZO1</i>, <i>RHAG</i>, <i>SH2B3</i>, and <i>VHL</i> genes. One <i>NF1</i> pathogenic, one <i>BPGM</i> likely pathogenic, and six variants of undetermined significance were detected.</p><h3 data-test=\\\"abstract-sub-heading\\\">Conclusion</h3><p>Somatic and germline mutations were identified in 36.4% and 33.3 % of the <i>JAK2</i>-unmutated group; most variants had unknown clinical significance. 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Diagnostic Approaches to Investigate JAK2-Unmutated Erythrocytosis Based on a Single Tertiary Center Experience
Introduction
Erythrocytosis is attributed to various clinical and molecular factors. Many cases of JAK2-unmutated erythrocytosis remain undiagnosed. We investigated the characteristics and causes of JAK2-unmutated erythrocytosis.
Methods
We assessed the clinical and laboratory results of patients with erythrocytosis without JAK2 mutations and performed targeted next-generation sequencing (NGS) panels for somatic and germline mutations.
Results
In total, 117 patients with JAK2-unmutated erythrocytosis were included. The median hemoglobin and hematocrit levels were 17.9 g/dL and 53.4%, respectively. Erythropoietin levels were not below the reference range. Thrombotic events were reported in 17 patients (14.5%). Among JAK2-unmutated patients, 44 had undergone targeted panel sequencing consisting of myeloid neoplasm-related genes, and 16 had one or more reportable variants in ASXL1 (5/44), TET2, CALR, FLT3, and SH2B3 (2/44). Additional testing for germline causes revealed eight variants in seven genes in eight patients, including NF1, BPGM, EPAS1, PIEZO1, RHAG, SH2B3, and VHL genes. One NF1 pathogenic, one BPGM likely pathogenic, and six variants of undetermined significance were detected.
Conclusion
Somatic and germline mutations were identified in 36.4% and 33.3 % of the JAK2-unmutated group; most variants had unknown clinical significance. Not all genetic causes have been identified; comprehensive diagnostic approaches are crucial for identifying the cause of erythrocytosis.
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Molecular Diagnosis & Therapy welcomes current opinion articles on emerging or contentious issues, comprehensive narrative reviews, systematic reviews (as outlined by the PRISMA statement), original research articles (including short communications) and letters to the editor. All manuscripts are subject to peer review by international experts.
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