A Prospective Cohort Study to Define the Clinical Features and Outcome of Lung Cancers Harboring HER2 Aberration in Japan (HER2-CS STUDY)

Kiichiro Ninomiya; Tae Hata; Hiroshige Yoshioka; Kadoaki Ohashi; Akihiro Bessho; Shinobu Hosokawa; Nobuhisa Ishikawa; Masahiro Yamasaki; T. Shibayama; Keisuke Aoe; Toshiyuki Kozuki; Shingo Harita; Yutaka Ueda; T. Murakami; Nobukazu Fujimoto; Hiroyuki Yanai; Shinichi Toyooka; Minoru Takata; Katsuyuki Hotta; Katsuyuki Kiura; K. Gemba; G. Ikeda; M. Yasugi; E. Kurimoto; K. Nakano; T. Moritaka; K. Inoue; S. Miyoshi; N. Hamaguchi; R. Ito; Y. Sano; I. Takata; A. Mitani; T. Nishisaka; H. Shoda; A. Nishida; S. Tamamoto; K. Fujitaka; T. Masuda; S. Miyamoto; N. Hattori; K. Sugimoto; S. Fujii; Y. Ueda; M. Sakugawa; N. Fukamatsu; Y. Ogata; S. Bandoh; N. Kanaji; N. Takigawa; H. Yamane; N. Ochi; Y. Honda; M. Oka; M. Kittaka; T. Kubota; A. Yokoyama; T. Yokoyama; E. Sato; Y. Shiota; N. Horita; T. Kanematsu; Y. Awaya; A. Nakamasu; I. Murakami; S. Kuyama; K. Kudo; T. Tamura; T. Umeno; D. Morichika; K. Fujiwara; K. Sato; D. Harada; N. Nogami; K. Nishii; Y. Fuchimoto; T. Kishimoto; H. Kawai; K. Watanabe; K. Tokumo; T. Isobe; Y. Tsubata; M. Inoue; H. Ichikawa; Y. Nishioka; M. Hanibuchi; H. Goto; T. Sumikawa; M. Kodani; H. Suyama; H. Makino; N. Kinosita; E. Shimizu; H. Obata; H. Ikegami; K. Chikamori; T. Maeda; T. Kishino; H. Kamei; H. Ueoka; Y. Kunihiro; T. Kobayashi; K. Ueda; M. Hayashi; M. Kamiya; J. Murakami; Akiko Sato; E. Ichihara; Toshio Kubo; Takashi Ninomiya; T. Hirata; Daisuke Minami; Yuka Kato; H. Higo; G. Makimoto; Y. Toyota; N. Oda; M. Nakanishi; H. Kayatani; S. Senoo; H. Kano; H. Watanabe; T. Ando; T. Nakasuka; N. Hara; J. Itano; H. Nakashima; M. Tabata

doi:10.1016/j.chest.2019.01.011

A Prospective Cohort Study to Define the Clinical Features and Outcome of Lung Cancers Harboring HER2 Aberration in Japan (HER2-CS STUDY)

Kiichiro Ninomiya, Tae Hata, Hiroshige Yoshioka, Kadoaki Ohashi, Akihiro Bessho, Shinobu Hosokawa, Nobuhisa Ishikawa, Masahiro Yamasaki, T. Shibayama, Keisuke Aoe, Toshiyuki Kozuki, Shingo Harita, Yutaka Ueda, T. Murakami, Nobukazu Fujimoto, Hiroyuki Yanai, Shinichi Toyooka, Minoru Takata, Katsuyuki Hotta, Katsuyuki KiuraK. Gemba, G. Ikeda, M. Yasugi, E. Kurimoto, K. Nakano, T. Moritaka, K. Inoue, S. Miyoshi, N. Hamaguchi, R. Ito, Y. Sano, I. Takata, A. Mitani, T. Nishisaka, H. Shoda, A. Nishida, S. Tamamoto, K. Fujitaka, T. Masuda, S. Miyamoto, N. Hattori, K. Sugimoto, S. Fujii, Y. Ueda, M. Sakugawa, N. Fukamatsu, Y. Ogata, S. Bandoh, N. Kanaji, N. Takigawa, H. Yamane, N. Ochi, Y. Honda, M. Oka, M. Kittaka, T. Kubota, A. Yokoyama, T. Yokoyama, E. Sato, Y. Shiota, N. Horita, T. Kanematsu, Y. Awaya, A. Nakamasu, I. Murakami, S. Kuyama, K. Kudo, T. Tamura, T. Umeno, D. Morichika, K. Fujiwara, K. Sato, D. Harada, N. Nogami, K. Nishii, Y. Fuchimoto, T. Kishimoto, H. Kawai, K. Watanabe, K. Tokumo, T. Isobe, Y. Tsubata, M. Inoue, H. Ichikawa, Y. Nishioka, M. Hanibuchi, H. Goto, T. Sumikawa, M. Kodani, H. Suyama, H. Makino, N. Kinosita, E. Shimizu, H. Obata, H. Ikegami, K. Chikamori, T. Maeda, T. Kishino, H. Kamei, H. Ueoka, Y. Kunihiro, T. Kobayashi, K. Ueda, M. Hayashi, M. Kamiya, J. Murakami, Akiko Sato, E. Ichihara, Toshio Kubo, Takashi Ninomiya, T. Hirata, Daisuke Minami, Yuka Kato, H. Higo, G. Makimoto, Y. Toyota, N. Oda, M. Nakanishi, H. Kayatani, S. Senoo, H. Kano, H. Watanabe, T. Ando, T. Nakasuka, N. Hara, J. Itano, H. Nakashima, M. Tabata

研究成果 › 査読

25 被引用数 (Scopus)

抄録

Background: Human epidermal growth factor 2 (HER2) is a potential driver oncogene. Although HER2-targeted precision therapy has been tested in non-small cell lung cancer (NSCLC), the demographic characteristics of HER2-positive NSCLC have not been systematically defined. Methods: Patients with pathologically confirmed stage IIIB/IV or recurrent NSCLC, Eastern Cooperative Oncology Group performance status 0 to 2, were prospectively registered. HER2 immunohistochemistry (IHC) and fluorescence in situ hybridization (FISH) assays were performed to screen patients. HER2 mutations were identified by using direct gene sequencing. The aim of this study was to clarify the frequency, characteristics, and outcome of HER2-positive NSCLC. HER2 was defined as positive if the tumor harbored IHC3+, IHC2+/FISH+, or exon 20 insertion mutations. Results: Of the 1,126 tumors screened, 34 (3.0%) were IHC3+, and 34 (3.0%) were IHC2+/FISH+. Among the 724 epidermal growth factor receptor wild-type tumors, 21 (2.9%) were HER2-mutant tumors, including A775-G776insYVMA (n = 15). Interestingly, the IHC3+ tumors and mutant tumors were entirely exclusive. Female patients had HER2-mutant tumors more frequently, whereas both IHC3+ and IHC2+/FISH+ tumors were detected more often in male subjects and smokers. Patients with an HER2-aberrant tumor had a significantly worse prognosis than those with epidermal growth factor receptor-positive and anaplastic lymphoma kinase-positive tumors, possibly due to the low proportion that received HER2-targeted therapies (n = 15 [26%]) and low response rates of 0% and 14% in patients with HER2-overexpressing and HER2-mutant tumors, respectively. Conclusions: This prospective large-scale cohort study is the first to show comprehensively the frequency and clinical demographic characteristics of those with HER2-positive advanced lung tumors in detail, providing critical historical data for future drug development against HER2-positive NSCLC. Future treatment strategies would be developed stratified according to the types of HER2 aberrations. Trial Registry: UMIN Registration No. 000017003; URL: https://upload.umin.ac.jp/cgi-open-bin/ctr_e/ctr_view.cgi?recptno=R000019691

本文言語	English
ページ（範囲）	357-366
ページ数	10
ジャーナル	Chest
巻	156
号	2
DOI	https://doi.org/10.1016/j.chest.2019.01.011
出版ステータス	Published - 8月 2019

ASJC Scopus subject areas

呼吸器内科
集中医療医学
循環器および心血管医学

UN SDG

この成果は、次の持続可能な開発目標に貢献しています

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10.1016/j.chest.2019.01.011

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引用スタイル

Ninomiya, K., Hata, T., Yoshioka, H., Ohashi, K., Bessho, A., Hosokawa, S., Ishikawa, N., Yamasaki, M., Shibayama, T., Aoe, K., Kozuki, T., Harita, S., Ueda, Y., Murakami, T., Fujimoto, N., Yanai, H., Toyooka, S., Takata, M., Hotta, K., ... Tabata, M. (2019). A Prospective Cohort Study to Define the Clinical Features and Outcome of Lung Cancers Harboring HER2 Aberration in Japan (HER2-CS STUDY). Chest, 156(2), 357-366. https://doi.org/10.1016/j.chest.2019.01.011

Ninomiya, K, Hata, T, Yoshioka, H, Ohashi, K, Bessho, A, Hosokawa, S, Ishikawa, N, Yamasaki, M, Shibayama, T, Aoe, K, Kozuki, T, Harita, S, Ueda, Y, Murakami, T, Fujimoto, N, Yanai, H , Toyooka, S, Takata, M, Hotta, K , Kiura, K, Gemba, K, Ikeda, G, Yasugi, M, Kurimoto, E, Nakano, K, Moritaka, T, Inoue, K, Miyoshi, S, Hamaguchi, N, Ito, R, Sano, Y, Takata, I, Mitani, A, Nishisaka, T, Shoda, H, Nishida, A, Tamamoto, S, Fujitaka, K, Masuda, T, Miyamoto, S, Hattori, N, Sugimoto, K, Fujii, S, Ueda, Y, Sakugawa, M, Fukamatsu, N, Ogata, Y, Bandoh, S, Kanaji, N, Takigawa, N, Yamane, H, Ochi, N, Honda, Y, Oka, M, Kittaka, M, Kubota, T, Yokoyama, A, Yokoyama, T, Sato, E, Shiota, Y, Horita, N, Kanematsu, T, Awaya, Y, Nakamasu, A, Murakami, I, Kuyama, S, Kudo, K, Tamura, T, Umeno, T, Morichika, D, Fujiwara, K, Sato, K, Harada, D, Nogami, N, Nishii, K, Fuchimoto, Y, Kishimoto, T, Kawai, H, Watanabe, K, Tokumo, K, Isobe, T, Tsubata, Y, Inoue, M, Ichikawa, H, Nishioka, Y, Hanibuchi, M, Goto, H, Sumikawa, T, Kodani, M, Suyama, H, Makino, H, Kinosita, N, Shimizu, E, Obata, H, Ikegami, H, Chikamori, K, Maeda, T, Kishino, T, Kamei, H, Ueoka, H, Kunihiro, Y, Kobayashi, T, Ueda, K, Hayashi, M, Kamiya, M, Murakami, J, Sato, A, Ichihara, E, Kubo, T, Ninomiya, T, Hirata, T, Minami, D, Kato, Y, Higo, H , Makimoto, G, Toyota, Y, Oda, N, Nakanishi, M, Kayatani, H, Senoo, S, Kano, H, Watanabe, H, Ando, T, Nakasuka, T, Hara, N, Itano, J, Nakashima, H & Tabata, M 2019, 'A Prospective Cohort Study to Define the Clinical Features and Outcome of Lung Cancers Harboring HER2 Aberration in Japan (HER2-CS STUDY)', Chest, vol. 156, no. 2, pp. 357-366. https://doi.org/10.1016/j.chest.2019.01.011

@article{951b6497ea7c4e0d82d35d2641aff198,

title = "A Prospective Cohort Study to Define the Clinical Features and Outcome of Lung Cancers Harboring HER2 Aberration in Japan (HER2-CS STUDY)",

abstract = "Background: Human epidermal growth factor 2 (HER2) is a potential driver oncogene. Although HER2-targeted precision therapy has been tested in non-small cell lung cancer (NSCLC), the demographic characteristics of HER2-positive NSCLC have not been systematically defined. Methods: Patients with pathologically confirmed stage IIIB/IV or recurrent NSCLC, Eastern Cooperative Oncology Group performance status 0 to 2, were prospectively registered. HER2 immunohistochemistry (IHC) and fluorescence in situ hybridization (FISH) assays were performed to screen patients. HER2 mutations were identified by using direct gene sequencing. The aim of this study was to clarify the frequency, characteristics, and outcome of HER2-positive NSCLC. HER2 was defined as positive if the tumor harbored IHC3+, IHC2+/FISH+, or exon 20 insertion mutations. Results: Of the 1,126 tumors screened, 34 (3.0%) were IHC3+, and 34 (3.0%) were IHC2+/FISH+. Among the 724 epidermal growth factor receptor wild-type tumors, 21 (2.9%) were HER2-mutant tumors, including A775-G776insYVMA (n = 15). Interestingly, the IHC3+ tumors and mutant tumors were entirely exclusive. Female patients had HER2-mutant tumors more frequently, whereas both IHC3+ and IHC2+/FISH+ tumors were detected more often in male subjects and smokers. Patients with an HER2-aberrant tumor had a significantly worse prognosis than those with epidermal growth factor receptor-positive and anaplastic lymphoma kinase-positive tumors, possibly due to the low proportion that received HER2-targeted therapies (n = 15 [26%]) and low response rates of 0% and 14% in patients with HER2-overexpressing and HER2-mutant tumors, respectively. Conclusions: This prospective large-scale cohort study is the first to show comprehensively the frequency and clinical demographic characteristics of those with HER2-positive advanced lung tumors in detail, providing critical historical data for future drug development against HER2-positive NSCLC. Future treatment strategies would be developed stratified according to the types of HER2 aberrations. Trial Registry: UMIN Registration No. 000017003; URL: https://upload.umin.ac.jp/cgi-open-bin/ctr_e/ctr_view.cgi?recptno=R000019691",

keywords = "fluorescence in situ hybridization, human epidermal growth factor 2, immunohistochemistry, mutation, non-small cell lung cancer",

author = "Kiichiro Ninomiya and Tae Hata and Hiroshige Yoshioka and Kadoaki Ohashi and Akihiro Bessho and Shinobu Hosokawa and Nobuhisa Ishikawa and Masahiro Yamasaki and T. Shibayama and Keisuke Aoe and Toshiyuki Kozuki and Shingo Harita and Yutaka Ueda and T. Murakami and Nobukazu Fujimoto and Hiroyuki Yanai and Shinichi Toyooka and Minoru Takata and Katsuyuki Hotta and Katsuyuki Kiura and K. Gemba and G. Ikeda and M. Yasugi and E. Kurimoto and K. Nakano and T. Moritaka and K. Inoue and S. Miyoshi and N. Hamaguchi and R. Ito and Y. Sano and I. Takata and A. Mitani and T. Nishisaka and H. Shoda and A. Nishida and S. Tamamoto and K. Fujitaka and T. Masuda and S. Miyamoto and N. Hattori and K. Sugimoto and S. Fujii and Y. Ueda and M. Sakugawa and N. Fukamatsu and Y. Ogata and S. Bandoh and N. Kanaji and N. Takigawa and H. Yamane and N. Ochi and Y. Honda and M. Oka and M. Kittaka and T. Kubota and A. Yokoyama and T. Yokoyama and E. Sato and Y. Shiota and N. Horita and T. Kanematsu and Y. Awaya and A. Nakamasu and I. Murakami and S. Kuyama and K. Kudo and T. Tamura and T. Umeno and D. Morichika and K. Fujiwara and K. Sato and D. Harada and N. Nogami and K. Nishii and Y. Fuchimoto and T. Kishimoto and H. Kawai and K. Watanabe and K. Tokumo and T. Isobe and Y. Tsubata and M. Inoue and H. Ichikawa and Y. Nishioka and M. Hanibuchi and H. Goto and T. Sumikawa and M. Kodani and H. Suyama and H. Makino and N. Kinosita and E. Shimizu and H. Obata and H. Ikegami and K. Chikamori and T. Maeda and T. Kishino and H. Kamei and H. Ueoka and Y. Kunihiro and T. Kobayashi and K. Ueda and M. Hayashi and M. Kamiya and J. Murakami and Akiko Sato and E. Ichihara and Toshio Kubo and Takashi Ninomiya and T. Hirata and Daisuke Minami and Yuka Kato and H. Higo and G. Makimoto and Y. Toyota and N. Oda and M. Nakanishi and H. Kayatani and S. Senoo and H. Kano and H. Watanabe and T. Ando and T. Nakasuka and N. Hara and J. Itano and H. Nakashima and M. Tabata",

note = "Funding Information: Other contributions: The authors acknowledge and thank the investigators, coordinators, and all others involved who have contributed to this study. This study has been conducted with support from the LC-SCRUM group (S. Matsumoto and K. Goto) and the Center for Innovative Clinical Medicine, Okayama University Hospital (N. Kondoh, M. Fukata, S. Kuroda, S. Sugihara, N. Nakabayashi, N. Hiramatsu, S. Hinotsu, K. Zama, W. Ishii, Y. Ohe, C. Harada, M. Yoshida, K, Kamikawa, K. Shikata and J. Sakurai). Funding Information: Author contributions: The Steering Committee comprised K. H. K. O. K. N. S. T. and K. K.; and H. Yanai and M. T. were advisers to the HER2 aberration analysis. K. O. K. H. T. H. K. N. H. K. and K. K. also took part in the trial design and trial set-up; and K. O. K. H. K. N. and K. K. calculated the sample size. All authors contributed to the writing of the protocol. K. N. H. Yanai, and M. T. analyzed the data; T. H. H. Yoshioka, K. O. A. B. S. Hosokawa, N. I. M. Y. T. S. K. A. T. K. S. Harita, Y. U. T. M. and N. F. were responsible for acquisition of the data; S. T. and K. K. interpreted the results; and K. H. interpreted the results and drafted the manuscript. All authors critically reviewed the manuscript for important intellectual content. All authors have reviewed the version of the manuscript to be submitted and are in agreement with its content and submission. Financial/nonfinancial disclosures: The authors have reported to CHEST the following: K. N. has received honoraria outside the current work from Bristol-Myers Squibb and Merck Sharp & Dohme. K. O. has received research funding outside of the current work from Boehringer-Ingelheim and Novartis Pharmaceuticals Japan. K. H. has received honoraria outside the current work from AstraZeneca, Ono Pharmaceutical, Astellas, Novartis, Bristol-Myers Squibb, Merck Sharp & Dohme, Eli Lilly Japan, Daiichi-Sankyo Pharmaceutical, Boehringer-Ingelheim, Nihon Kayaku, Taiho Pharmaceutical, and Chugai Pharmaceutical. K. H. also has received research funding outside of the current work from AstraZeneca, Boehringer-Ingelheim, Ono Pharmaceutical, Astellas, Novartis, Bristol-Myers Squibb, Eli Lilly Japan, Merck Sharp & Dohme, and Chugai Pharmaceutical. K. K. has received honoraria outside the current work from Eli Lilly Japan, Nihon Kayaku, AstraZeneca, Daiichi-Sankyo Pharmaceutical, Chugai Pharmaceutical, Taiho Pharmaceutical, and Sanofi-Aventis. None declared (T. H. H. Yoshioka, K. O. A. B. S. Hosokawa, N. I. M. Y. T. S. K. A. T. K. S. Harita, Y. U. T. M. N. F. H. Yanai, S. T. M. T.). Role of sponsors: The sponsor had no role in the design of the study, the collection and analysis of the data, or the preparation of the manuscript. HER2-CS Network Collaborators: This study has been conducted with dedicated contributions from the following: the HER2-CS Study group (K. Gemba, G. Ikeda, M. Yasugi, E. Kurimoto, K. Nakano [Chugoku Central Hospital], T. Moritaka, K. Inoue [Ehime Prefectural Central Hospital], S. Miyoshi, N. Hamaguchi, R. Ito, Y. Sano [Ehime University Hospital], I. Takata, A. Mitani [Fukuyama City Hospital], T. Nishisaka, H. Shoda, A. Nishida, S. Tamamoto [Hiroshima Prefectural Hospital], K. Fujitaka, T. Masuda, S. Miyamoto, N. Hattori [Hiroshima University Hospital], K. Sugimoto, S. Fujii, Y. Ueda [Japanese Red Cross Kobe Hospital], M. Sakugawa, N. Fukamatsu, Y. Ogata [Japanese Red Cross Okayama Hospital], S. Bandoh, N. Kanaji [Kagawa University Hospital], N. Takigawa, H. Yamane, N. Ochi, Y. Honda [Kawasaki Hospital], M. Oka, M. Kittaka [Kawasaki Medical School Hospital], T. Kubota, A. Yokoyama [Kochi Medical School Hospital], T. Yokoyama, E. Sato [Kurashiki Central Hospital], Y. Shiota, N. Horita [Kure Kyosai Hospital], T. Kanematsu [Matsuyama Red Cross Hospital], Y. Awaya, A. Nakamasu, Y. Sano [Miyoshi Central Hospital], I. Murakami [NHO Higashi-Hiroshima Medical Center], S. Kuyama, K. Kudo, T. Tamura, T. Umeno, D. Morichika [NHO Iwakuni Medical Center], K. Fujiwara, K. Sato [NHO Okayama Medical Center], D. Harada, N. Nogami [NHO Shikoku Cancer Center], K. Nishii [Okayama Health Foundation Hospital], Y. Fuchimoto, T. Kishimoto [Okayama Rosai Hospital], H. Kawai, K. Watanabe [Okayama Saiseikai General Hospital], K. Tokumo [Onomichi General Hospital], T. Isobe, Y. Tsubata [Shimane University School of Medicine], M. Inoue [Shimonoseki City Hospital], H. Ichikawa [Takamatsu Hospital], Y. Nishioka, M. Hanibuchi, H. Goto [Tokushima University Hospital], T. Sumikawa [Tottori Prefectural Central Hospital], M. Kodani, H. Suyama, H. Makino, Y. Ueda, N. Kinosita, E. Shimizu [Tottori University Hospital], H. Obata, H. Ikegami [Yamaguchi-ken Saiseikai Shimonoseki General Hospital], K. Chikamori, T. Maeda, T. Kishino, H. Kamei, H. Ueoka [NHO Yamaguchi-Ube Medical Center], Y. Kunihiro, T. Kobayashi, K. Ueda, M. Hayashi, M. Kamiya, J. Murakami [Yamaguchi University Hospital], A. Sato, E. Ichihara, T. Kubo, T. Ninomiya, T. Hirata, D. Minami, Y. Kato, H. Higo, G. Makimoto, Y. Toyota, N. Oda, M. Nakanishi, H. Kayatani, K. Nishii, S. Senoo, H. Kano, H. Watanabe, T. Ando, T. Nakasuka, N. Hara, J. Itano, H. Nakashima, and M. Tabata [Okayama University Hospital]). Other contributions: The authors acknowledge and thank the investigators, coordinators, and all others involved who have contributed to this study. This study has been conducted with support from the LC-SCRUM group (S. Matsumoto and K. Goto) and the Center for Innovative Clinical Medicine, Okayama University Hospital (N. Kondoh, M. Fukata, S. Kuroda, S. Sugihara, N. Nakabayashi, N. Hiramatsu, S. Hinotsu, K. Zama, W. Ishii, Y. Ohe, C. Harada, M. Yoshida, K, Kamikawa, K. Shikata and J. Sakurai). Additional information: The e-Appendix, e-Figures, and e-Tables can be found in the Supplemental Materials section of the online article. FUNDING/SUPPORT: This research was supported by a specific grant from the Japan Agency for Medical Research and Development, which is funded by the Japanese government. Publisher Copyright: {\textcopyright} 2019 American College of Chest Physicians",

year = "2019",

month = aug,

doi = "10.1016/j.chest.2019.01.011",

language = "English",

volume = "156",

pages = "357--366",

journal = "Diseases of the chest",

issn = "0012-3692",

publisher = "American College of Chest Physicians",

number = "2",

}

TY - JOUR

T1 - A Prospective Cohort Study to Define the Clinical Features and Outcome of Lung Cancers Harboring HER2 Aberration in Japan (HER2-CS STUDY)

AU - Ninomiya, Kiichiro

AU - Hata, Tae

AU - Yoshioka, Hiroshige

AU - Ohashi, Kadoaki

AU - Bessho, Akihiro

AU - Hosokawa, Shinobu

AU - Ishikawa, Nobuhisa

AU - Yamasaki, Masahiro

AU - Shibayama, T.

AU - Aoe, Keisuke

AU - Kozuki, Toshiyuki

AU - Harita, Shingo

AU - Ueda, Yutaka

AU - Murakami, T.

AU - Fujimoto, Nobukazu

AU - Yanai, Hiroyuki

AU - Toyooka, Shinichi

AU - Takata, Minoru

AU - Hotta, Katsuyuki

AU - Kiura, Katsuyuki

AU - Gemba, K.

AU - Ikeda, G.

AU - Yasugi, M.

AU - Kurimoto, E.

AU - Nakano, K.

AU - Moritaka, T.

AU - Inoue, K.

AU - Miyoshi, S.

AU - Hamaguchi, N.

AU - Ito, R.

AU - Sano, Y.

AU - Takata, I.

AU - Mitani, A.

AU - Nishisaka, T.

AU - Shoda, H.

AU - Nishida, A.

AU - Tamamoto, S.

AU - Fujitaka, K.

AU - Masuda, T.

AU - Miyamoto, S.

AU - Hattori, N.

AU - Sugimoto, K.

AU - Fujii, S.

AU - Ueda, Y.

AU - Sakugawa, M.

AU - Fukamatsu, N.

AU - Ogata, Y.

AU - Bandoh, S.

AU - Kanaji, N.

AU - Takigawa, N.

AU - Yamane, H.

AU - Ochi, N.

AU - Honda, Y.

AU - Oka, M.

AU - Kittaka, M.

AU - Kubota, T.

AU - Yokoyama, A.

AU - Yokoyama, T.

AU - Sato, E.

AU - Shiota, Y.

AU - Horita, N.

AU - Kanematsu, T.

AU - Awaya, Y.

AU - Nakamasu, A.

AU - Murakami, I.

AU - Kuyama, S.

AU - Kudo, K.

AU - Tamura, T.

AU - Umeno, T.

AU - Morichika, D.

AU - Fujiwara, K.

AU - Sato, K.

AU - Harada, D.

AU - Nogami, N.

AU - Nishii, K.

AU - Fuchimoto, Y.

AU - Kishimoto, T.

AU - Kawai, H.

AU - Watanabe, K.

AU - Tokumo, K.

AU - Isobe, T.

AU - Tsubata, Y.

AU - Inoue, M.

AU - Ichikawa, H.

AU - Nishioka, Y.

AU - Hanibuchi, M.

AU - Goto, H.

AU - Sumikawa, T.

AU - Kodani, M.

AU - Suyama, H.

AU - Makino, H.

AU - Kinosita, N.

AU - Shimizu, E.

AU - Obata, H.

AU - Ikegami, H.

AU - Chikamori, K.

AU - Maeda, T.

AU - Kishino, T.

AU - Kamei, H.

AU - Ueoka, H.

AU - Kunihiro, Y.

AU - Kobayashi, T.

AU - Ueda, K.

AU - Hayashi, M.

AU - Kamiya, M.

AU - Murakami, J.

AU - Sato, Akiko

AU - Ichihara, E.

AU - Kubo, Toshio

AU - Ninomiya, Takashi

AU - Hirata, T.

AU - Minami, Daisuke

AU - Kato, Yuka

AU - Higo, H.

AU - Makimoto, G.

AU - Toyota, Y.

AU - Oda, N.

AU - Nakanishi, M.

AU - Kayatani, H.

AU - Senoo, S.

AU - Kano, H.

AU - Watanabe, H.

AU - Ando, T.

AU - Nakasuka, T.

AU - Hara, N.

AU - Itano, J.

AU - Nakashima, H.

AU - Tabata, M.

N1 - Funding Information: Other contributions: The authors acknowledge and thank the investigators, coordinators, and all others involved who have contributed to this study. This study has been conducted with support from the LC-SCRUM group (S. Matsumoto and K. Goto) and the Center for Innovative Clinical Medicine, Okayama University Hospital (N. Kondoh, M. Fukata, S. Kuroda, S. Sugihara, N. Nakabayashi, N. Hiramatsu, S. Hinotsu, K. Zama, W. Ishii, Y. Ohe, C. Harada, M. Yoshida, K, Kamikawa, K. Shikata and J. Sakurai). Funding Information: Author contributions: The Steering Committee comprised K. H. K. O. K. N. S. T. and K. K.; and H. Yanai and M. T. were advisers to the HER2 aberration analysis. K. O. K. H. T. H. K. N. H. K. and K. K. also took part in the trial design and trial set-up; and K. O. K. H. K. N. and K. K. calculated the sample size. All authors contributed to the writing of the protocol. K. N. H. Yanai, and M. T. analyzed the data; T. H. H. Yoshioka, K. O. A. B. S. Hosokawa, N. I. M. Y. T. S. K. A. T. K. S. Harita, Y. U. T. M. and N. F. were responsible for acquisition of the data; S. T. and K. K. interpreted the results; and K. H. interpreted the results and drafted the manuscript. All authors critically reviewed the manuscript for important intellectual content. All authors have reviewed the version of the manuscript to be submitted and are in agreement with its content and submission. Financial/nonfinancial disclosures: The authors have reported to CHEST the following: K. N. has received honoraria outside the current work from Bristol-Myers Squibb and Merck Sharp & Dohme. K. O. has received research funding outside of the current work from Boehringer-Ingelheim and Novartis Pharmaceuticals Japan. K. H. has received honoraria outside the current work from AstraZeneca, Ono Pharmaceutical, Astellas, Novartis, Bristol-Myers Squibb, Merck Sharp & Dohme, Eli Lilly Japan, Daiichi-Sankyo Pharmaceutical, Boehringer-Ingelheim, Nihon Kayaku, Taiho Pharmaceutical, and Chugai Pharmaceutical. K. H. also has received research funding outside of the current work from AstraZeneca, Boehringer-Ingelheim, Ono Pharmaceutical, Astellas, Novartis, Bristol-Myers Squibb, Eli Lilly Japan, Merck Sharp & Dohme, and Chugai Pharmaceutical. K. K. has received honoraria outside the current work from Eli Lilly Japan, Nihon Kayaku, AstraZeneca, Daiichi-Sankyo Pharmaceutical, Chugai Pharmaceutical, Taiho Pharmaceutical, and Sanofi-Aventis. None declared (T. H. H. Yoshioka, K. O. A. B. S. Hosokawa, N. I. M. Y. T. S. K. A. T. K. S. Harita, Y. U. T. M. N. F. H. Yanai, S. T. M. T.). Role of sponsors: The sponsor had no role in the design of the study, the collection and analysis of the data, or the preparation of the manuscript. HER2-CS Network Collaborators: This study has been conducted with dedicated contributions from the following: the HER2-CS Study group (K. Gemba, G. Ikeda, M. Yasugi, E. Kurimoto, K. Nakano [Chugoku Central Hospital], T. Moritaka, K. Inoue [Ehime Prefectural Central Hospital], S. Miyoshi, N. Hamaguchi, R. Ito, Y. Sano [Ehime University Hospital], I. Takata, A. Mitani [Fukuyama City Hospital], T. Nishisaka, H. Shoda, A. Nishida, S. Tamamoto [Hiroshima Prefectural Hospital], K. Fujitaka, T. Masuda, S. Miyamoto, N. Hattori [Hiroshima University Hospital], K. Sugimoto, S. Fujii, Y. Ueda [Japanese Red Cross Kobe Hospital], M. Sakugawa, N. Fukamatsu, Y. Ogata [Japanese Red Cross Okayama Hospital], S. Bandoh, N. Kanaji [Kagawa University Hospital], N. Takigawa, H. Yamane, N. Ochi, Y. Honda [Kawasaki Hospital], M. Oka, M. Kittaka [Kawasaki Medical School Hospital], T. Kubota, A. Yokoyama [Kochi Medical School Hospital], T. Yokoyama, E. Sato [Kurashiki Central Hospital], Y. Shiota, N. Horita [Kure Kyosai Hospital], T. Kanematsu [Matsuyama Red Cross Hospital], Y. Awaya, A. Nakamasu, Y. Sano [Miyoshi Central Hospital], I. Murakami [NHO Higashi-Hiroshima Medical Center], S. Kuyama, K. Kudo, T. Tamura, T. Umeno, D. Morichika [NHO Iwakuni Medical Center], K. Fujiwara, K. Sato [NHO Okayama Medical Center], D. Harada, N. Nogami [NHO Shikoku Cancer Center], K. Nishii [Okayama Health Foundation Hospital], Y. Fuchimoto, T. Kishimoto [Okayama Rosai Hospital], H. Kawai, K. Watanabe [Okayama Saiseikai General Hospital], K. Tokumo [Onomichi General Hospital], T. Isobe, Y. Tsubata [Shimane University School of Medicine], M. Inoue [Shimonoseki City Hospital], H. Ichikawa [Takamatsu Hospital], Y. Nishioka, M. Hanibuchi, H. Goto [Tokushima University Hospital], T. Sumikawa [Tottori Prefectural Central Hospital], M. Kodani, H. Suyama, H. Makino, Y. Ueda, N. Kinosita, E. Shimizu [Tottori University Hospital], H. Obata, H. Ikegami [Yamaguchi-ken Saiseikai Shimonoseki General Hospital], K. Chikamori, T. Maeda, T. Kishino, H. Kamei, H. Ueoka [NHO Yamaguchi-Ube Medical Center], Y. Kunihiro, T. Kobayashi, K. Ueda, M. Hayashi, M. Kamiya, J. Murakami [Yamaguchi University Hospital], A. Sato, E. Ichihara, T. Kubo, T. Ninomiya, T. Hirata, D. Minami, Y. Kato, H. Higo, G. Makimoto, Y. Toyota, N. Oda, M. Nakanishi, H. Kayatani, K. Nishii, S. Senoo, H. Kano, H. Watanabe, T. Ando, T. Nakasuka, N. Hara, J. Itano, H. Nakashima, and M. Tabata [Okayama University Hospital]). Other contributions: The authors acknowledge and thank the investigators, coordinators, and all others involved who have contributed to this study. This study has been conducted with support from the LC-SCRUM group (S. Matsumoto and K. Goto) and the Center for Innovative Clinical Medicine, Okayama University Hospital (N. Kondoh, M. Fukata, S. Kuroda, S. Sugihara, N. Nakabayashi, N. Hiramatsu, S. Hinotsu, K. Zama, W. Ishii, Y. Ohe, C. Harada, M. Yoshida, K, Kamikawa, K. Shikata and J. Sakurai). Additional information: The e-Appendix, e-Figures, and e-Tables can be found in the Supplemental Materials section of the online article. FUNDING/SUPPORT: This research was supported by a specific grant from the Japan Agency for Medical Research and Development, which is funded by the Japanese government. Publisher Copyright: © 2019 American College of Chest Physicians

PY - 2019/8

Y1 - 2019/8

N2 - Background: Human epidermal growth factor 2 (HER2) is a potential driver oncogene. Although HER2-targeted precision therapy has been tested in non-small cell lung cancer (NSCLC), the demographic characteristics of HER2-positive NSCLC have not been systematically defined. Methods: Patients with pathologically confirmed stage IIIB/IV or recurrent NSCLC, Eastern Cooperative Oncology Group performance status 0 to 2, were prospectively registered. HER2 immunohistochemistry (IHC) and fluorescence in situ hybridization (FISH) assays were performed to screen patients. HER2 mutations were identified by using direct gene sequencing. The aim of this study was to clarify the frequency, characteristics, and outcome of HER2-positive NSCLC. HER2 was defined as positive if the tumor harbored IHC3+, IHC2+/FISH+, or exon 20 insertion mutations. Results: Of the 1,126 tumors screened, 34 (3.0%) were IHC3+, and 34 (3.0%) were IHC2+/FISH+. Among the 724 epidermal growth factor receptor wild-type tumors, 21 (2.9%) were HER2-mutant tumors, including A775-G776insYVMA (n = 15). Interestingly, the IHC3+ tumors and mutant tumors were entirely exclusive. Female patients had HER2-mutant tumors more frequently, whereas both IHC3+ and IHC2+/FISH+ tumors were detected more often in male subjects and smokers. Patients with an HER2-aberrant tumor had a significantly worse prognosis than those with epidermal growth factor receptor-positive and anaplastic lymphoma kinase-positive tumors, possibly due to the low proportion that received HER2-targeted therapies (n = 15 [26%]) and low response rates of 0% and 14% in patients with HER2-overexpressing and HER2-mutant tumors, respectively. Conclusions: This prospective large-scale cohort study is the first to show comprehensively the frequency and clinical demographic characteristics of those with HER2-positive advanced lung tumors in detail, providing critical historical data for future drug development against HER2-positive NSCLC. Future treatment strategies would be developed stratified according to the types of HER2 aberrations. Trial Registry: UMIN Registration No. 000017003; URL: https://upload.umin.ac.jp/cgi-open-bin/ctr_e/ctr_view.cgi?recptno=R000019691

AB - Background: Human epidermal growth factor 2 (HER2) is a potential driver oncogene. Although HER2-targeted precision therapy has been tested in non-small cell lung cancer (NSCLC), the demographic characteristics of HER2-positive NSCLC have not been systematically defined. Methods: Patients with pathologically confirmed stage IIIB/IV or recurrent NSCLC, Eastern Cooperative Oncology Group performance status 0 to 2, were prospectively registered. HER2 immunohistochemistry (IHC) and fluorescence in situ hybridization (FISH) assays were performed to screen patients. HER2 mutations were identified by using direct gene sequencing. The aim of this study was to clarify the frequency, characteristics, and outcome of HER2-positive NSCLC. HER2 was defined as positive if the tumor harbored IHC3+, IHC2+/FISH+, or exon 20 insertion mutations. Results: Of the 1,126 tumors screened, 34 (3.0%) were IHC3+, and 34 (3.0%) were IHC2+/FISH+. Among the 724 epidermal growth factor receptor wild-type tumors, 21 (2.9%) were HER2-mutant tumors, including A775-G776insYVMA (n = 15). Interestingly, the IHC3+ tumors and mutant tumors were entirely exclusive. Female patients had HER2-mutant tumors more frequently, whereas both IHC3+ and IHC2+/FISH+ tumors were detected more often in male subjects and smokers. Patients with an HER2-aberrant tumor had a significantly worse prognosis than those with epidermal growth factor receptor-positive and anaplastic lymphoma kinase-positive tumors, possibly due to the low proportion that received HER2-targeted therapies (n = 15 [26%]) and low response rates of 0% and 14% in patients with HER2-overexpressing and HER2-mutant tumors, respectively. Conclusions: This prospective large-scale cohort study is the first to show comprehensively the frequency and clinical demographic characteristics of those with HER2-positive advanced lung tumors in detail, providing critical historical data for future drug development against HER2-positive NSCLC. Future treatment strategies would be developed stratified according to the types of HER2 aberrations. Trial Registry: UMIN Registration No. 000017003; URL: https://upload.umin.ac.jp/cgi-open-bin/ctr_e/ctr_view.cgi?recptno=R000019691

KW - fluorescence in situ hybridization

KW - human epidermal growth factor 2

KW - immunohistochemistry

KW - mutation

KW - non-small cell lung cancer

UR - http://www.scopus.com/inward/record.url?scp=85065055094&partnerID=8YFLogxK

UR - http://www.scopus.com/inward/citedby.url?scp=85065055094&partnerID=8YFLogxK

U2 - 10.1016/j.chest.2019.01.011

DO - 10.1016/j.chest.2019.01.011

M3 - Article

C2 - 31072612

AN - SCOPUS:85065055094

SN - 0012-3692

VL - 156

SP - 357

EP - 366

JO - Diseases of the chest

JF - Diseases of the chest

IS - 2

ER -