Novel DDX41 variants in Thai patients with myeloid neoplasms

© 2019, Japanese Society of Hematology. Germline DDX41 mutations were recently reported to cause MDS/AML and donor-derived leukemia after transplantation. While previously described in Western countries, DDX41 variants have not been reported in a Southeast Asian population. We performed targeted seq...

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Main Authors: Chantana Polprasert, June Takeda, Pimjai Niparuck, Thanawat Rattanathammethee, Arunrat Pirunsarn, Amornchai Suksusut, Sirorat Kobbuaklee, Kitsada Wudhikarn, Panisinee Lawasut, Sunisa Kongkiatkamon, Suporn Chuncharunee, Kritanan Songserm, Prasit Phowthongkum, Udomsak Bunworasate, Yasuhito Nannya, Kenichi Yoshida, Hideki Makishima, Seishi Ogawa, Ponlapat Rojnuckarin
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Published: 2020
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http://cmuir.cmu.ac.th/jspui/handle/6653943832/68498
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spelling th-cmuir.6653943832-684982020-04-02T15:28:31Z Novel DDX41 variants in Thai patients with myeloid neoplasms Chantana Polprasert June Takeda Pimjai Niparuck Thanawat Rattanathammethee Arunrat Pirunsarn Amornchai Suksusut Sirorat Kobbuaklee Kitsada Wudhikarn Panisinee Lawasut Sunisa Kongkiatkamon Suporn Chuncharunee Kritanan Songserm Prasit Phowthongkum Udomsak Bunworasate Yasuhito Nannya Kenichi Yoshida Hideki Makishima Seishi Ogawa Ponlapat Rojnuckarin Medicine © 2019, Japanese Society of Hematology. Germline DDX41 mutations were recently reported to cause MDS/AML and donor-derived leukemia after transplantation. While previously described in Western countries, DDX41 variants have not been reported in a Southeast Asian population. We performed targeted sequencing of blood or bone marrow samples from 109 Thai patients with myeloid malignancies. Among the 109 patients (75 MDS, 8 MPN, 11 MDS/MPN and 15 AML), the most frequent mutations were in ASXL1 (17.4%), TET2 (16.5%) and SRSF2 (12.8%), respectively. DDX41 variants were detectable in six (5.5%) cases. Four patients exhibited three presumable germline DDX41 mutations: p.S21fs (n = 2), p.F235fs (n = 1), and p.R339H (n = 1). While p.S21fs was previously reported in myeloid neoplasm, the latter two variants have not been described. Two of these cases harbored concomitant probable germline/somatic DDX41 mutations (p.S21fs/p.R525H and p.R339H/p.K494T), while the other two patients carried only somatic mutations (p.R525H and p.F438L). The p.K494T and p.F438L variants have not been previously reported. In patients with DDX41 alterations, the diagnoses were MDS with excess blasts (4), secondary AML (1) and low-risk MDS (1). In conclusion, we identified DDX41 variants in Thai patients with myeloid malignancies in which these variants could be used to assess predisposition to MDS in Southeast Asia. 2020-04-02T15:28:31Z 2020-04-02T15:28:31Z 2020-02-01 Journal 18653774 09255710 2-s2.0-85075040765 10.1007/s12185-019-02770-3 https://www.scopus.com/inward/record.uri?partnerID=HzOxMe3b&scp=85075040765&origin=inward http://cmuir.cmu.ac.th/jspui/handle/6653943832/68498
institution Chiang Mai University
building Chiang Mai University Library
country Thailand
collection CMU Intellectual Repository
topic Medicine
spellingShingle Medicine
Chantana Polprasert
June Takeda
Pimjai Niparuck
Thanawat Rattanathammethee
Arunrat Pirunsarn
Amornchai Suksusut
Sirorat Kobbuaklee
Kitsada Wudhikarn
Panisinee Lawasut
Sunisa Kongkiatkamon
Suporn Chuncharunee
Kritanan Songserm
Prasit Phowthongkum
Udomsak Bunworasate
Yasuhito Nannya
Kenichi Yoshida
Hideki Makishima
Seishi Ogawa
Ponlapat Rojnuckarin
Novel DDX41 variants in Thai patients with myeloid neoplasms
description © 2019, Japanese Society of Hematology. Germline DDX41 mutations were recently reported to cause MDS/AML and donor-derived leukemia after transplantation. While previously described in Western countries, DDX41 variants have not been reported in a Southeast Asian population. We performed targeted sequencing of blood or bone marrow samples from 109 Thai patients with myeloid malignancies. Among the 109 patients (75 MDS, 8 MPN, 11 MDS/MPN and 15 AML), the most frequent mutations were in ASXL1 (17.4%), TET2 (16.5%) and SRSF2 (12.8%), respectively. DDX41 variants were detectable in six (5.5%) cases. Four patients exhibited three presumable germline DDX41 mutations: p.S21fs (n = 2), p.F235fs (n = 1), and p.R339H (n = 1). While p.S21fs was previously reported in myeloid neoplasm, the latter two variants have not been described. Two of these cases harbored concomitant probable germline/somatic DDX41 mutations (p.S21fs/p.R525H and p.R339H/p.K494T), while the other two patients carried only somatic mutations (p.R525H and p.F438L). The p.K494T and p.F438L variants have not been previously reported. In patients with DDX41 alterations, the diagnoses were MDS with excess blasts (4), secondary AML (1) and low-risk MDS (1). In conclusion, we identified DDX41 variants in Thai patients with myeloid malignancies in which these variants could be used to assess predisposition to MDS in Southeast Asia.
format Journal
author Chantana Polprasert
June Takeda
Pimjai Niparuck
Thanawat Rattanathammethee
Arunrat Pirunsarn
Amornchai Suksusut
Sirorat Kobbuaklee
Kitsada Wudhikarn
Panisinee Lawasut
Sunisa Kongkiatkamon
Suporn Chuncharunee
Kritanan Songserm
Prasit Phowthongkum
Udomsak Bunworasate
Yasuhito Nannya
Kenichi Yoshida
Hideki Makishima
Seishi Ogawa
Ponlapat Rojnuckarin
author_facet Chantana Polprasert
June Takeda
Pimjai Niparuck
Thanawat Rattanathammethee
Arunrat Pirunsarn
Amornchai Suksusut
Sirorat Kobbuaklee
Kitsada Wudhikarn
Panisinee Lawasut
Sunisa Kongkiatkamon
Suporn Chuncharunee
Kritanan Songserm
Prasit Phowthongkum
Udomsak Bunworasate
Yasuhito Nannya
Kenichi Yoshida
Hideki Makishima
Seishi Ogawa
Ponlapat Rojnuckarin
author_sort Chantana Polprasert
title Novel DDX41 variants in Thai patients with myeloid neoplasms
title_short Novel DDX41 variants in Thai patients with myeloid neoplasms
title_full Novel DDX41 variants in Thai patients with myeloid neoplasms
title_fullStr Novel DDX41 variants in Thai patients with myeloid neoplasms
title_full_unstemmed Novel DDX41 variants in Thai patients with myeloid neoplasms
title_sort novel ddx41 variants in thai patients with myeloid neoplasms
publishDate 2020
url https://www.scopus.com/inward/record.uri?partnerID=HzOxMe3b&scp=85075040765&origin=inward
http://cmuir.cmu.ac.th/jspui/handle/6653943832/68498
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