TY - JOUR
T1 - Clinical utility of target capture-based panel sequencing in hematological malignancies
T2 - A multicenter feasibility study
AU - Yasuda, Takahiko
AU - Sanada, Masashi
AU - Nishijima, Dai
AU - Kanamori, Takashi
AU - Iijima, Yuka
AU - Hattori, Hiroyoshi
AU - Saito, Akiko
AU - Miyoshi, Hiroaki
AU - Ishikawa, Yuichi
AU - Asou, Norio
AU - Usuki, Kensuke
AU - Hirabayashi, Shinsuke
AU - Kato, Motohiro
AU - Ri, Masaki
AU - Handa, Hiroshi
AU - Ishida, Tadao
AU - Shibayama, Hirohiko
AU - Abe, Masahiro
AU - Iriyama, Chisako
AU - Karube, Kennosuke
AU - Nishikori, Momoko
AU - Ohshima, Koichi
AU - Kataoka, Keisuke
AU - Yoshida, Kenichi
AU - Shiraishi, Yuichi
AU - Goto, Hiroaki
AU - Adachi, Souichi
AU - Kobayashi, Ryoji
AU - Kiyoi, Hitoshi
AU - Miyazaki, Yasushi
AU - Ogawa, Seishi
AU - Kurahashi, Hiroki
AU - Yokoyama, Hisayuki
AU - Manabe, Atsushi
AU - Iida, Shinsuke
AU - Tomita, Akihiro
AU - Horibe, Keizo
N1 - Publisher Copyright:
© 2020 The Authors. Cancer Science published by John Wiley & Sons Australia, Ltd on behalf of Japanese Cancer Association
PY - 2020/9/1
Y1 - 2020/9/1
N2 - Although next-generation sequencing-based panel testing is well practiced in the field of cancer medicine for the identification of target molecules in solid tumors, the clinical utility and clinical issues surrounding panel testing in hematological malignancies have yet to be fully evaluated. We conducted a multicenter prospective clinical sequencing study to verify the feasibility of a panel test for hematological tumors, including acute myeloid leukemia, acute lymphoblastic leukemia, multiple myeloma, and diffuse large B-cell lymphoma. Out of 96 eligible patients, 79 patients (82%) showed potentially actionable findings, based on the clinical sequencing assays. We identified that genetic alterations with a strong clinical significance were found at a higher frequency in terms of diagnosis (n = 60; 63%) and prognosis (n = 61; 64%) than in terms of therapy (n = 8; 8%). Three patients who harbored a germline mutation in either DDX41 (n = 2) or BRCA2 (n = 1) were provided with genetic counseling. At 6 mo after sequencing, clinical actions based on the diagnostic (n = 5) or prognostic (n = 3) findings were reported, but no patients were enrolled in a clinical trial or received targeted therapies based on the sequencing results. These results suggest that panel testing for hematological malignancies would be feasible given the availability of useful diagnostic and prognostic information. This study is registered with the UMIN Clinical Trial Registry (UMIN000029879, multiple myeloma; UMIN000031343, adult acute myeloid leukemia; UMIN000033144, diffuse large B-cell lymphoma; and UMIN000034243, childhood leukemia).
AB - Although next-generation sequencing-based panel testing is well practiced in the field of cancer medicine for the identification of target molecules in solid tumors, the clinical utility and clinical issues surrounding panel testing in hematological malignancies have yet to be fully evaluated. We conducted a multicenter prospective clinical sequencing study to verify the feasibility of a panel test for hematological tumors, including acute myeloid leukemia, acute lymphoblastic leukemia, multiple myeloma, and diffuse large B-cell lymphoma. Out of 96 eligible patients, 79 patients (82%) showed potentially actionable findings, based on the clinical sequencing assays. We identified that genetic alterations with a strong clinical significance were found at a higher frequency in terms of diagnosis (n = 60; 63%) and prognosis (n = 61; 64%) than in terms of therapy (n = 8; 8%). Three patients who harbored a germline mutation in either DDX41 (n = 2) or BRCA2 (n = 1) were provided with genetic counseling. At 6 mo after sequencing, clinical actions based on the diagnostic (n = 5) or prognostic (n = 3) findings were reported, but no patients were enrolled in a clinical trial or received targeted therapies based on the sequencing results. These results suggest that panel testing for hematological malignancies would be feasible given the availability of useful diagnostic and prognostic information. This study is registered with the UMIN Clinical Trial Registry (UMIN000029879, multiple myeloma; UMIN000031343, adult acute myeloid leukemia; UMIN000033144, diffuse large B-cell lymphoma; and UMIN000034243, childhood leukemia).
KW - clinical sequencing
KW - feasibility study
KW - hematological malignancy
KW - panel testing
KW - potentially actionable finding
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U2 - 10.1111/cas.14552
DO - 10.1111/cas.14552
M3 - Article
C2 - 32619037
AN - SCOPUS:85088047813
SN - 1347-9032
VL - 111
SP - 3367
EP - 3378
JO - Cancer science
JF - Cancer science
IS - 9
ER -