Your search keyword '"Koyama, Takafumi"' showing total 9 results

1. Comprehensive Genomic Assessment of Advanced-Stage GI Stromal Tumors Using the Japanese National Center for Cancer Genomics and Advanced Therapeutics Database.

Author

Fujii, Hiroyuki, Hirano, Hidekazu, Shiraishi, Kouya, Shoji, Hirokazu, Hirose, Toshiharu, Okita, Natsuko, Takashima, Atsuo, Koyama, Takafumi, and Kato, Ken

Subjects

EPIDERMAL growth factor receptors, HOMOLOGOUS recombination, DATABASES, JAPANESE people, INDIVIDUALIZED medicine, GASTROINTESTINAL stromal tumors

Abstract

PURPOSE: Clinical utility of comprehensive genomic profiling (CGP) for precision medicine has become evident. Although there are several reports on the genomic landscape of GI stromal tumors (GISTs), large-scale data specific to GIST are limited, especially in Asia. Additionally, the applicability of molecular-targeted agents identified using CGP has not been extensively examined. We investigated the status of genomic alterations in Japanese patients with advanced GISTs using the National Center for Cancer Genomics and Advanced Therapeutics (C-CAT) database to identify novel treatment strategies and drug development. MATERIALS AND METHODS: We retrospectively reviewed the clinical and CGP data of patients with advanced-stage GIST registered in the C-CAT database to assess the genomic landscape and potential actionable alterations. RESULTS: Data from 144 patients were reviewed. Oncogenic alterations were detected frequently in KIT (78%), CDKN2A (37%), CDKN2B (29%), RB1 (11%), STK11 (10%), TP53 (9%), PDGFRA (6%), and SDHB (6%). Loss of CDKN2A / CDKN2B was only observed in KIT/PDGFRA -mutated GISTs, while alterations in SDHA/SDHB were only detected in KIT/PDGFRA wild-type GISTs. Among 119 KIT/PDGFRA -mutated GISTs, 95 (80%) had oncogenic genomic alterations and 29 (24%) had actionable alterations, excluding KIT and PDGFRA. However, among 25 KIT/PDGFRA wild-type GISTs, 22 (88%) had oncogenic alterations and 11 (44%) had actionable alterations. Representative candidate drugs for genome-matched therapies in KIT/PDGFRA -mutated and wild-type GISTs were as follows: pembrolizumab for tumor mutation burden–high in one and two patients, respectively; poly-adenosine diphosphate ribose polymerase inhibitors for alterations related to homologous recombination deficiency in 12 and one patient, respectively; NTRK inhibitor for ETV6-NTRK3 fusion in one with KIT/PDGFRA wild-type GIST; and human epidermal growth factor receptor 2-antibody-drug conjugate in one with KIT/PDGFRA -mutated GIST. CONCLUSION: This study highlights the genomic landscape of advanced GISTs and the important role of CGP in identifying rational molecular-targeted therapeutic options. [ABSTRACT FROM AUTHOR]

Published

2024

2. Efficacy and safety of olomorasib (LY3537982), a second-generation KRAS G12C inhibitor (G12Ci), in combination with pembrolizumab in patients with KRAS G12C-mutant advanced NSCLC.

Author

Fujiwara, Yutaka, Burns, Timothy F., Dragnev, Konstantin H., Murciano-Goroff, Yonina R., Lee, Dae Ho, Hollebecque, Antoine, Koyama, Takafumi, Cassier, Philippe Alexandre, Italiano, Antoine, Heist, Rebecca Suk, Han, Ji-Youn, Deming, Dustin A., Spira, Alexander I., Sabari, Joshua K., Chisamore, Michael Jon, Fink, Aaron Alan, Chen, Aaron, Willard, Melinda D., Oxnard, Geoffrey R., and Ammakkanavar, Natraj Reddy

Published

2024

3. Efficacy and safety of LY3537982, a potent and highly selective KRAS G12C inhibitor in KRAS G12C-mutant GI cancers: Results from a phase 1 study.

Author

Hollebecque, Antoine, Kuboki, Yasutoshi, Murciano-Goroff, Yonina R., Yaeger, Rona, Cassier, Philippe Alexandre, Heist, Rebecca Suk, Fujiwara, Yutaka, Deming, Dustin A., Ammakkanavar, Natraj, Patnaik, Amita, Shimizu, Toshio, Call, Justin, Han, Sae-Won, Fink, Aaron Alan, Chen, Aaron, Willard, Melinda D, Balar, Arjun Vasant, and Koyama, Takafumi

Published

2024

4. Comprehensive genomic profiling of advanced anal adenocarcinoma.

Author

Ogura, Nozomu, Hirano, Hidekazu, Shiraishi, Kouya, Fujii, Hiroyuki, Hirose, Toshiharu, Shoji, Hirokazu, Okita, Natsuko Tsuda, Takashima, Atsuo, Koyama, Takafumi, and Kato, Ken

Published

2024

5. Genomic characterization of unresectable/recurrent early-onset gastric cancer by comprehensive genomic profiling tests.

Author

Matsuguma, Kunihito, Hirano, Hidekazu, Fujii, Hiroyuki, Shiraishi, Kouya, Shoji, Hirokazu, Hirose, Toshiharu, Okita, Natsuko Tsuda, Takashima, Atsuo, Koyama, Takafumi, and Kato, Ken

Published

2024

6. Pediatric Precision Medicine at the National Cancer Center Japan: Prospective Genomic Study of Pediatric Patients with Cancer as Part of the TOP-GEAR Project.

Author

Tao, Kayoko, Yamazaki, Fumito, Kubo, Takashi, Sunami, Kuniko, Kumamoto, Tadashi, Arakawa, Ayumu, Sugiyama, Masanaka, Watanabe, Yuko, Nakajima, Miho, Shirakawa, Nami, Tanimura, Kazuki, Koyama, Takafumi, Hirata, Makoto, Sudo, Kazuki, Tanabe, Noriko, Watanabe, Tomoko, Yoshida, Teruhiko, Kitami, Mayuko, Yoshida, Akihiko, and Yatabe, Yasushi

Subjects

CHILD patients, PEDIATRICS, CANCER patients, CHILDHOOD cancer, INDIVIDUALIZED medicine

Abstract

PURPOSE: This single-center, prospective molecular profiling study characterizes genomic alterations and identifies therapeutic targets in advanced pediatric solid tumors. METHODS: As part of the TOP-GEAR (Trial of Onco-Panel for Gene profiling to Estimate both Adverse events and Response by cancer treatment) project at the National Cancer Center (NCC), Japan, we enrolled pediatric patients with a refractory or recurrent disease during August 2016-December 2021 and performed genomic analysis of matched tumors and blood using originally developed cancer gene panels, NCC Oncopanel (ver. 4.0) and NCC Oncopanel Ped (ver. 1.0). RESULTS: Of 142 patients (age, 1-28 years) enrolled, 128 (90%) were evaluable for genomic analysis; 76 (59%) patients harbored at least one reportable somatic or germline alteration. The tumor samples were collected during the initial diagnosis in 65 (51%) patients, after treatment initiation in 11 (9%) patients, and upon either disease progression or relapse in 52 (41%) patients. The leading altered gene was TP53 , followed by MYCN , MYC, CDKN2A , and CDK4. The commonly affected molecular processes were transcription, cell-cycle regulation, epigenetic modifiers, and RAS/mitogen-activated protein kinase signaling. Twelve (9%) patients carried pathogenic germline variants in cancer-predisposing genes. Potentially actionable findings were identified in 40 (31%) patients; to date, 13 (10%) patients have received the recommended therapy on the basis of their genomic profiles. Although four patients had access to targeted therapy through clinical trials, the agents were used in nine patients in an off-label setting. CONCLUSION: The implementation of genomic medicine has furthered our understanding of tumor biology and provided new therapeutic strategies. However, the paucity of proposed agents limits the full potential of actionability, emphasizing the significance of facilitating access to targeted cancer therapies. The NCC Japan TOP-GEAR study highlights the importance of diligent optimization in pediatric cancer genomic medicine. [ABSTRACT FROM AUTHOR]

Published

2023

7. Trends in the needs and clinical utility of comprehensive genomic profiling test in rare cancers before and after the National Health Insurance coverage in Japan.

Author

Sanomachi, Tomomi, Okuma, Hitomi Sumiyoshi, Mizuno, Takaaki, Kojima, Yuki, Maejima, Aiko, Narita, Yoshitaka, Ohe, Yuichiro, Yamazaki, Naoya, Kawai, Akira, Okusaka, Takuji, Kato, Ken, Sunami, Kuniko, Koyama, Takafumi, Kohno, Takashi, Ichikawa, Hitoshi, Kakishima, Hiroki, Yamamoto, Noboru, Yatabe, Yasushi, and Yonemori, Kan

Published

2023

8. Impact of patient travel time on disparities in precision oncology clinical trials.

Author

Uehara, Yuji, Koyama, Takafumi, Katsuya, Yuki, Sato, Jun, and Yamamoto, Noboru

Published

2023

9. Exploratory novel biomarker and resistance mechanism of milademetan, an MDM2 inhibitor, in amplified MDM2 intimal sarcoma from an open-label phase 1b/2 trial (NCCH1806/MK004).

Author

Koyama, Takafumi, Shimizu, Toshio, Kojima, Yuki, Sudo, Kazuki, Okuma, Hitomi Sumiyoshi, Shimoi, Tatsunori, Ichikawa, Hitoshi, Kohsaka, Shinji, Yoshida, Akihiko, Matsui, Naoko, Nakamura, Kenichi, Yamamoto, Noboru, and Yonemori, Kan

Published

2023