A combination of TERT promoter mutation and MGMT methylation status predicts clinically relevant subgroups of newly diagnosed glioblastomas

Hideyuki Arita; Kai Yamasaki; Yuko Matsushita; Taishi Nakamura; Asanao Shimokawa; Hirokazu Takami; Shota Tanaka; Akitake Mukasa; Mitsuaki Shirahata; Saki Shimizu; Kaori Suzuki; Kuniaki Saito; Keiichi Kobayashi; Fumi Higuchi; Takeo Uzuka; Ryohei Otani; Kaoru Tamura; Kazutaka Sumita; Makoto Ohno; Yasuji Miyakita; Naoki Kagawa; Naoya Hashimoto; Ryusuke Hatae; Koji Yoshimoto; Naoki Shinojima; Hideo Nakamura; Yonehiro Kanemura; Yoshiko Okita; Manabu Kinoshita; Kenichi Ishibashi; Tomoko Shofuda; Yoshinori Kodama; Kanji Mori; Yusuke Tomogane; Junya Fukai; Koji Fujita; Yuzo Terakawa; Naohiro Tsuyuguchi; Shusuke Moriuchi; Masahiro Nonaka; Hiroyoshi Suzuki; Makoto Shibuya; Taketoshi Maehara; Nobuhito Saito; Motoo Nagane; Nobutaka Kawahara; Keisuke Ueki; Toshiki Yoshimine; Etsuo Miyaoka; Ryo Nishikawa; Takashi Komori; Yoshitaka Narita; Koichi Ichimura

doi:10.1186/s40478-016-0351-2

A combination of TERT promoter mutation and MGMT methylation status predicts clinically relevant subgroups of newly diagnosed glioblastomas

Hideyuki Arita, Kai Yamasaki, Yuko Matsushita, Taishi Nakamura, Asanao Shimokawa, Hirokazu Takami, Shota Tanaka, Akitake Mukasa, Mitsuaki Shirahata, Saki Shimizu, Kaori Suzuki, Kuniaki Saito, Keiichi Kobayashi, Fumi Higuchi, Takeo Uzuka, Ryohei Otani, Kaoru Tamura, Kazutaka Sumita, Makoto Ohno, Yasuji MiyakitaNaoki Kagawa, Naoya Hashimoto, Ryusuke Hatae, Koji Yoshimoto, Naoki Shinojima, Hideo Nakamura, Yonehiro Kanemura, Yoshiko Okita, Manabu Kinoshita, Kenichi Ishibashi, Tomoko Shofuda, Yoshinori Kodama, Kanji Mori, Yusuke Tomogane, Junya Fukai, Koji Fujita, Yuzo Terakawa, Naohiro Tsuyuguchi, Shusuke Moriuchi, Masahiro Nonaka, Hiroyoshi Suzuki, Makoto Shibuya, Taketoshi Maehara, Nobuhito Saito, Motoo Nagane, Nobutaka Kawahara, Keisuke Ueki, Toshiki Yoshimine, Etsuo Miyaoka, Ryo Nishikawa, Takashi Komori, Yoshitaka Narita, Koichi Ichimura

数学科

研究成果: Article › 査読

200 被引用数 (Scopus)

抄録

The prognostic impact of TERT mutations has been controversial in IDH-wild tumors, particularly in glioblastomas (GBM). The controversy may be attributable to presence of potential confounding factors such as MGMT methylation status or patients' treatment. This study aimed to evaluate the impact of TERT status on patient outcome in association with various factors in a large series of adult diffuse gliomas. We analyzed a total of 951 adult diffuse gliomas from two cohorts (Cohort 1, n = 758; Cohort 2, n = 193) for IDH1/2, 1p/19q, and TERT promoter status. The combined IDH/TERT classification divided Cohort 1 into four molecular groups with distinct outcomes. The overall survival (OS) was the shortest in IDH wild-type/TERT mutated groups, which mostly consisted of GBMs (P < 0.0001). To investigate the association between TERT mutations and MGMT methylation on survival of patients with GBM, samples from a combined cohort of 453 IDH-wild-type GBM cases treated with radiation and temozolomide were analyzed. A multivariate Cox regression model revealed that the interaction between TERT and MGMT was significant for OS (P = 0.0064). Compared with TERT mutant-MGMT unmethylated GBMs, the hazard ratio (HR) for OS incorporating the interaction was the lowest in the TERT mutant-MGMT methylated GBM (HR, 0.266), followed by the TERT wild-type-MGMT methylated (HR, 0.317) and the TERT wild-type-MGMT unmethylated GBMs (HR, 0.542). Thus, patients with TERT mutant-MGMT unmethylated GBM have the poorest prognosis. Our findings suggest that a combination of IDH, TERT, and MGMT refines the classification of grade II-IV diffuse gliomas.

本文言語	English
ページ（範囲）	79
ページ数	1
ジャーナル	Acta neuropathologica communications
巻	4
号	1
DOI	https://doi.org/10.1186/s40478-016-0351-2
出版ステータス	Published - 8 8月 2016

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10.1186/s40478-016-0351-2

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引用スタイル

Arita, H., Yamasaki, K., Matsushita, Y., Nakamura, T., Shimokawa, A., Takami, H., Tanaka, S., Mukasa, A., Shirahata, M., Shimizu, S., Suzuki, K., Saito, K., Kobayashi, K., Higuchi, F., Uzuka, T., Otani, R., Tamura, K., Sumita, K., Ohno, M., ... Ichimura, K. (2016). A combination of TERT promoter mutation and MGMT methylation status predicts clinically relevant subgroups of newly diagnosed glioblastomas. Acta neuropathologica communications, 4(1), 79. https://doi.org/10.1186/s40478-016-0351-2

@article{ab4f9ea20cc54dcd831120f0c69f63f0,

title = "A combination of TERT promoter mutation and MGMT methylation status predicts clinically relevant subgroups of newly diagnosed glioblastomas",

abstract = "The prognostic impact of TERT mutations has been controversial in IDH-wild tumors, particularly in glioblastomas (GBM). The controversy may be attributable to presence of potential confounding factors such as MGMT methylation status or patients' treatment. This study aimed to evaluate the impact of TERT status on patient outcome in association with various factors in a large series of adult diffuse gliomas. We analyzed a total of 951 adult diffuse gliomas from two cohorts (Cohort 1, n = 758; Cohort 2, n = 193) for IDH1/2, 1p/19q, and TERT promoter status. The combined IDH/TERT classification divided Cohort 1 into four molecular groups with distinct outcomes. The overall survival (OS) was the shortest in IDH wild-type/TERT mutated groups, which mostly consisted of GBMs (P < 0.0001). To investigate the association between TERT mutations and MGMT methylation on survival of patients with GBM, samples from a combined cohort of 453 IDH-wild-type GBM cases treated with radiation and temozolomide were analyzed. A multivariate Cox regression model revealed that the interaction between TERT and MGMT was significant for OS (P = 0.0064). Compared with TERT mutant-MGMT unmethylated GBMs, the hazard ratio (HR) for OS incorporating the interaction was the lowest in the TERT mutant-MGMT methylated GBM (HR, 0.266), followed by the TERT wild-type-MGMT methylated (HR, 0.317) and the TERT wild-type-MGMT unmethylated GBMs (HR, 0.542). Thus, patients with TERT mutant-MGMT unmethylated GBM have the poorest prognosis. Our findings suggest that a combination of IDH, TERT, and MGMT refines the classification of grade II-IV diffuse gliomas. ",

keywords = "1p19q, Glioblastoma, Glioma, IDH1/2, Molecular classification, Prognostic factor, TERT, Temozolomide",

author = "Hideyuki Arita and Kai Yamasaki and Yuko Matsushita and Taishi Nakamura and Asanao Shimokawa and Hirokazu Takami and Shota Tanaka and Akitake Mukasa and Mitsuaki Shirahata and Saki Shimizu and Kaori Suzuki and Kuniaki Saito and Keiichi Kobayashi and Fumi Higuchi and Takeo Uzuka and Ryohei Otani and Kaoru Tamura and Kazutaka Sumita and Makoto Ohno and Yasuji Miyakita and Naoki Kagawa and Naoya Hashimoto and Ryusuke Hatae and Koji Yoshimoto and Naoki Shinojima and Hideo Nakamura and Yonehiro Kanemura and Yoshiko Okita and Manabu Kinoshita and Kenichi Ishibashi and Tomoko Shofuda and Yoshinori Kodama and Kanji Mori and Yusuke Tomogane and Junya Fukai and Koji Fujita and Yuzo Terakawa and Naohiro Tsuyuguchi and Shusuke Moriuchi and Masahiro Nonaka and Hiroyoshi Suzuki and Makoto Shibuya and Taketoshi Maehara and Nobuhito Saito and Motoo Nagane and Nobutaka Kawahara and Keisuke Ueki and Toshiki Yoshimine and Etsuo Miyaoka and Ryo Nishikawa and Takashi Komori and Yoshitaka Narita and Koichi Ichimura",

note = "Funding Information: HA received research grant from MSD K.K.. KI received research grant from SRL Inc., EPS and Chugai Pharmaceutical Co.Ltd. Funding Information: The authors also thank Ms. Ema Yoshioka and Mr. Daisuke Kanematsu (Institute for Clinical Research, Osaka National Hospital) for the generous assistance in genetic tests. This work was supported partially by JSPS KAKENHI Grant Number 25462283 (K.I.) and 26861171 (H.A.), and the Research award of Osaka Cancer Society (H.A.).",

year = "2016",

month = aug,

day = "8",

doi = "10.1186/s40478-016-0351-2",

language = "English",

volume = "4",

pages = "79",

journal = "Acta neuropathologica communications",

issn = "2051-5960",

publisher = "BioMed Central",

number = "1",

}

Arita, H, Yamasaki, K, Matsushita, Y, Nakamura, T, Shimokawa, A, Takami, H, Tanaka, S, Mukasa, A, Shirahata, M, Shimizu, S, Suzuki, K, Saito, K, Kobayashi, K, Higuchi, F, Uzuka, T, Otani, R, Tamura, K, Sumita, K, Ohno, M, Miyakita, Y, Kagawa, N, Hashimoto, N, Hatae, R, Yoshimoto, K, Shinojima, N, Nakamura, H, Kanemura, Y, Okita, Y, Kinoshita, M, Ishibashi, K, Shofuda, T, Kodama, Y, Mori, K, Tomogane, Y, Fukai, J, Fujita, K, Terakawa, Y, Tsuyuguchi, N, Moriuchi, S, Nonaka, M, Suzuki, H, Shibuya, M, Maehara, T, Saito, N, Nagane, M, Kawahara, N, Ueki, K, Yoshimine, T, Miyaoka, E, Nishikawa, R, Komori, T, Narita, Y & Ichimura, K 2016, 'A combination of TERT promoter mutation and MGMT methylation status predicts clinically relevant subgroups of newly diagnosed glioblastomas', Acta neuropathologica communications, vol. 4, no. 1, pp. 79. https://doi.org/10.1186/s40478-016-0351-2

TY - JOUR

T1 - A combination of TERT promoter mutation and MGMT methylation status predicts clinically relevant subgroups of newly diagnosed glioblastomas

AU - Arita, Hideyuki

AU - Yamasaki, Kai

AU - Matsushita, Yuko

AU - Nakamura, Taishi

AU - Shimokawa, Asanao

AU - Takami, Hirokazu

AU - Tanaka, Shota

AU - Mukasa, Akitake

AU - Shirahata, Mitsuaki

AU - Shimizu, Saki

AU - Suzuki, Kaori

AU - Saito, Kuniaki

AU - Kobayashi, Keiichi

AU - Higuchi, Fumi

AU - Uzuka, Takeo

AU - Otani, Ryohei

AU - Tamura, Kaoru

AU - Sumita, Kazutaka

AU - Ohno, Makoto

AU - Miyakita, Yasuji

AU - Kagawa, Naoki

AU - Hashimoto, Naoya

AU - Hatae, Ryusuke

AU - Yoshimoto, Koji

AU - Shinojima, Naoki

AU - Nakamura, Hideo

AU - Kanemura, Yonehiro

AU - Okita, Yoshiko

AU - Kinoshita, Manabu

AU - Ishibashi, Kenichi

AU - Shofuda, Tomoko

AU - Kodama, Yoshinori

AU - Mori, Kanji

AU - Tomogane, Yusuke

AU - Fukai, Junya

AU - Fujita, Koji

AU - Terakawa, Yuzo

AU - Tsuyuguchi, Naohiro

AU - Moriuchi, Shusuke

AU - Nonaka, Masahiro

AU - Suzuki, Hiroyoshi

AU - Shibuya, Makoto

AU - Maehara, Taketoshi

AU - Saito, Nobuhito

AU - Nagane, Motoo

AU - Kawahara, Nobutaka

AU - Ueki, Keisuke

AU - Yoshimine, Toshiki

AU - Miyaoka, Etsuo

AU - Nishikawa, Ryo

AU - Komori, Takashi

AU - Narita, Yoshitaka

AU - Ichimura, Koichi

N1 - Funding Information: HA received research grant from MSD K.K.. KI received research grant from SRL Inc., EPS and Chugai Pharmaceutical Co.Ltd. Funding Information: The authors also thank Ms. Ema Yoshioka and Mr. Daisuke Kanematsu (Institute for Clinical Research, Osaka National Hospital) for the generous assistance in genetic tests. This work was supported partially by JSPS KAKENHI Grant Number 25462283 (K.I.) and 26861171 (H.A.), and the Research award of Osaka Cancer Society (H.A.).

PY - 2016/8/8

Y1 - 2016/8/8

N2 - The prognostic impact of TERT mutations has been controversial in IDH-wild tumors, particularly in glioblastomas (GBM). The controversy may be attributable to presence of potential confounding factors such as MGMT methylation status or patients' treatment. This study aimed to evaluate the impact of TERT status on patient outcome in association with various factors in a large series of adult diffuse gliomas. We analyzed a total of 951 adult diffuse gliomas from two cohorts (Cohort 1, n = 758; Cohort 2, n = 193) for IDH1/2, 1p/19q, and TERT promoter status. The combined IDH/TERT classification divided Cohort 1 into four molecular groups with distinct outcomes. The overall survival (OS) was the shortest in IDH wild-type/TERT mutated groups, which mostly consisted of GBMs (P < 0.0001). To investigate the association between TERT mutations and MGMT methylation on survival of patients with GBM, samples from a combined cohort of 453 IDH-wild-type GBM cases treated with radiation and temozolomide were analyzed. A multivariate Cox regression model revealed that the interaction between TERT and MGMT was significant for OS (P = 0.0064). Compared with TERT mutant-MGMT unmethylated GBMs, the hazard ratio (HR) for OS incorporating the interaction was the lowest in the TERT mutant-MGMT methylated GBM (HR, 0.266), followed by the TERT wild-type-MGMT methylated (HR, 0.317) and the TERT wild-type-MGMT unmethylated GBMs (HR, 0.542). Thus, patients with TERT mutant-MGMT unmethylated GBM have the poorest prognosis. Our findings suggest that a combination of IDH, TERT, and MGMT refines the classification of grade II-IV diffuse gliomas.

AB - The prognostic impact of TERT mutations has been controversial in IDH-wild tumors, particularly in glioblastomas (GBM). The controversy may be attributable to presence of potential confounding factors such as MGMT methylation status or patients' treatment. This study aimed to evaluate the impact of TERT status on patient outcome in association with various factors in a large series of adult diffuse gliomas. We analyzed a total of 951 adult diffuse gliomas from two cohorts (Cohort 1, n = 758; Cohort 2, n = 193) for IDH1/2, 1p/19q, and TERT promoter status. The combined IDH/TERT classification divided Cohort 1 into four molecular groups with distinct outcomes. The overall survival (OS) was the shortest in IDH wild-type/TERT mutated groups, which mostly consisted of GBMs (P < 0.0001). To investigate the association between TERT mutations and MGMT methylation on survival of patients with GBM, samples from a combined cohort of 453 IDH-wild-type GBM cases treated with radiation and temozolomide were analyzed. A multivariate Cox regression model revealed that the interaction between TERT and MGMT was significant for OS (P = 0.0064). Compared with TERT mutant-MGMT unmethylated GBMs, the hazard ratio (HR) for OS incorporating the interaction was the lowest in the TERT mutant-MGMT methylated GBM (HR, 0.266), followed by the TERT wild-type-MGMT methylated (HR, 0.317) and the TERT wild-type-MGMT unmethylated GBMs (HR, 0.542). Thus, patients with TERT mutant-MGMT unmethylated GBM have the poorest prognosis. Our findings suggest that a combination of IDH, TERT, and MGMT refines the classification of grade II-IV diffuse gliomas.

KW - 1p19q

KW - Glioblastoma

KW - Glioma

KW - IDH1/2

KW - Molecular classification

KW - Prognostic factor

KW - TERT

KW - Temozolomide

UR - https://www.scopus.com/pages/publications/85031277957

U2 - 10.1186/s40478-016-0351-2

DO - 10.1186/s40478-016-0351-2

M3 - Article

C2 - 27503138

AN - SCOPUS:85031277957

SN - 2051-5960

VL - 4

SP - 79

JO - Acta neuropathologica communications

JF - Acta neuropathologica communications

IS - 1

ER -