Your search keyword '"10252462"' showing total 5 results

1. A case of Langerhans cell sarcoma on the scalp: Whole‐exome sequencing reveals a role of ultraviolet in the pathogenesis

Author

40742622, 90573676, 10252462, Katsuragawa, Hiroyuki, Yamada, Yosuke, Ishida, Yoshihiro, Kaku, Yo, Fujimoto, Masakazu, Kataoka, Tatsuki R., Haga, Hironori, 40742622, 90573676, 10252462, Katsuragawa, Hiroyuki, Yamada, Yosuke, Ishida, Yoshihiro, Kaku, Yo, Fujimoto, Masakazu, Kataoka, Tatsuki R., and Haga, Hironori

Abstract

Langerhans cell sarcoma (LCS) is a high‐grade neoplasm with overtly malignant cytological features and a Langerhans cell phenotype. The underlying genetic features are poorly understood, and only a few alterations, such as those of the MARK pathway‐related genes, CDKN2A and TP53 have been reported. Here we present a 70‐year‐old male with LCS on the scalp and pulmonary metastasis. The multinodular tumor, 3.0 cm in diameter, consisted of diffusely proliferated pleomorphic cells with numerous mitoses (53/10 HPFs). Immunohistochemically, the tumor cells were positive for CD1a, Langerin and PD‐L1, and the Ki‐67 labeling index was 50%. These pathological features were consistent with LCS, and were also observed in the metastatic tumor. Whole‐exome sequencing revealed that both the primary and metastatic tumors harbored a large number of mutations (>20 mutations/megabase), with deletion of CDKN2A and TP53 mutation, and highlighted that the mutational signature was predominantly characteristic of ultraviolet (UV) exposure (W = 0.828). Our results suggest, for the first time, that DNA damage by UV could accumulate in Langerhans cells and play a role in the pathogenesis of LCS. The high mutational burden and PD‐L1 expression in the tumor would provide a rationale for the use of immune checkpoint inhibitors for treatment of unresectable LCS.

Published

2020

2. Clinical sequencing using a next-generation sequencing-based multiplex gene assay in patients with advanced solid tumors

Author

70432416, 70749077, 00335283, 10329485, 00378639, 10252462, 90335266, 50252432, 20283666, 40360698, Kou, Tadayuki, Kanai, Masashi, Yamamoto, Yoshihiro, Kamada, Mayumi, Nakatsui, Masahiko, Sakuma, Tomohiro, Mochizuki, Hiroaki, Hiroshima, Akinori, Sugiyama, Aiko, Nakamura, Eijiro, Miyake, Hidehiko, Minamiguchi, Sachiko, Takaori, Kyoichi, Matsumoto, Shigemi, Haga, Hironori, Seno, Hiroshi, Kosugi, Shinji, Okuno, Yasushi, Muto, Manabu, 70432416, 70749077, 00335283, 10329485, 00378639, 10252462, 90335266, 50252432, 20283666, 40360698, Kou, Tadayuki, Kanai, Masashi, Yamamoto, Yoshihiro, Kamada, Mayumi, Nakatsui, Masahiko, Sakuma, Tomohiro, Mochizuki, Hiroaki, Hiroshima, Akinori, Sugiyama, Aiko, Nakamura, Eijiro, Miyake, Hidehiko, Minamiguchi, Sachiko, Takaori, Kyoichi, Matsumoto, Shigemi, Haga, Hironori, Seno, Hiroshi, Kosugi, Shinji, Okuno, Yasushi, and Muto, Manabu

Abstract

Advances in next-generation sequencing (NGS) technologies have enabled physicians to test for genomic alterations in multiple cancer-related genes at once in daily clinical practice. In April 2015, we introduced clinical sequencing using an NGS-based multiplex gene assay (OncoPrime) certified by the Clinical Laboratory Improvement Amendment. This assay covers the entire coding regions of 215 genes and the rearrangement of 17 frequently rearranged genes with clinical relevance in human cancers. The principal indications for the assay were cancers of unknown primary site, rare tumors, and any solid tumors that were refractory to standard chemotherapy. A total of 85 patients underwent testing with multiplex gene assay between April 2015 and July 2016. The most common solid tumor types tested were pancreatic (n = 19; 22.4%), followed by biliary tract (n = 14; 16.5%), and tumors of unknown primary site (n = 13; 15.3%). Samples from 80 patients (94.1%) were successfully sequenced. The median turnaround time was 40 days (range, 18–70 days). Potentially actionable mutations were identified in 69 of 80 patients (86.3%) and were most commonly found in TP53 (46.3%), KRAS (23.8%), APC (18.8%), STK11 (7.5%), and ATR (7.5%). Nine patients (13.0%) received a subsequent therapy based on the NGS assay results. Implementation of clinical sequencing using an NGS-based multiplex gene assay was feasible in the clinical setting and identified potentially actionable mutations in more than 80% of patients. Current challenges are to incorporate this genomic information into better therapeutic decision making.

Published

2017

3. Expression of Tim-1 in primary CNS lymphoma

Author

60378635, 50618014, 50378684, 80728270, 10252462, Kishimoto, Wataru, Nishikori, Momoko, Arima, Hiroshi, Miyoshi, Hiroaki, Sasaki, Yuya, Kitawaki, Toshio, Shirakawa, Kotaro, Kato, Takeharu, Imaizumi, Yoshitaka, Ishikawa, Takayuki, Ohno, Hitoshi, Haga, Hironori, Ohshima, Koichi, Takaori-Kondo, Akifumi, 60378635, 50618014, 50378684, 80728270, 10252462, Kishimoto, Wataru, Nishikori, Momoko, Arima, Hiroshi, Miyoshi, Hiroaki, Sasaki, Yuya, Kitawaki, Toshio, Shirakawa, Kotaro, Kato, Takeharu, Imaizumi, Yoshitaka, Ishikawa, Takayuki, Ohno, Hitoshi, Haga, Hironori, Ohshima, Koichi, and Takaori-Kondo, Akifumi

Abstract

Primary central nervous system lymphoma (PCNSL) is a distinct subtype of extranodal lymphoma with aggressive clinical course and poor outcome. As increased IL-10/IL-6 ratio is recognized in the cerebrospinal fluid (CSF) of PCNSL patients, we hypothesized that PCNSL might originate from a population of B cells with high IL-10-producing capacity, an equivalent of "regulatory B cells" in mice. We intended in this study to clarify whether Tim-1, a molecule known as a marker for regulatory B cells in mice, is expressed in PCNSL. By immunohistochemical analysis, Tim-1 was shown to be positive in as high as 54.2% of PCNSL (26 of 58 samples), while it was positive in 19.1% of systemic diffuse large B-cell lymphoma (DLBCL) samples (17 of 89 samples; P < 0.001). Tim-1 expression positively correlated with IL-10 expression in PCNSL (Cramer's V = 0.55, P < 0.001), and forced expression of Tim-1 in a PCNSL cell line resulted in increased IL-10 secretion, suggesting that Tim-1 is functionally linked with IL-10 production in PCNSL. Moreover, soluble Tim-1 was detectable in the CSF of PCNSL patients, and was suggested to parallel disease activity. In summary, PCNSL is characterized by frequent Tim-1 expression, and its soluble form in CSF may become a useful biomarker for PCNSL.

Published

2016

4. Association between epithelial-mesenchymal transition and cancer stemness and their effect on the prognosis of lung adenocarcinoma

Author

80378645, 10252462, 60252962, Sowa, Terumasa, Menju, Toshi, Sonobe, Makoto, Nakanishi, Takao, Shikuma, Kei, Imamura, Naoto, Motoyama, Hideki, Hijiya, Kyoko, Aoyama, Akihiro, Chen, Fengshi, Sato, Toshihiko, Kobayashi, Masashi, Yoshizawa, Akihiko, Haga, Hironori, Sozu, Takashi, Date, Hiroshi, 80378645, 10252462, 60252962, Sowa, Terumasa, Menju, Toshi, Sonobe, Makoto, Nakanishi, Takao, Shikuma, Kei, Imamura, Naoto, Motoyama, Hideki, Hijiya, Kyoko, Aoyama, Akihiro, Chen, Fengshi, Sato, Toshihiko, Kobayashi, Masashi, Yoshizawa, Akihiko, Haga, Hironori, Sozu, Takashi, and Date, Hiroshi

Abstract

The epithelial-mesenchymal transition (EMT) and cancer stemness (CS) are reported to be pivotal phenomena involved in metastasis, recurrence, and drug-resistance in lung cancer; however, their effects on tumor malignancy in clinical settings are not completely understood. The mutual association between these factors also remains elusive and are worthy of investigation. The purpose of this study was to elucidate the association between EMT and CS, and their effect on the prognosis of patients with lung adenocarcinoma. A total of 239 lung adenocarcinoma specimens were collected from patients who had undergone surgery at Kyoto University Hospital from January 2001 to December 2007. Both EMT (E-cadherin, vimentin) and CS (CD133, CD44, aldehyde dehydrogenase) markers were analyzed through immunostaining of tumor specimens. The association between EMT and CS as well as the patients' clinical information was integrated and statistically analyzed. The molecular expression of E-cadherin, vimentin, and CD133 were significantly correlated with prognosis (P = 0.003, P = 0.005, and P < 0.001). A negative correlation was found between E-cadherin and vimentin expression (P < 0.001), whereas, a positive correlation was found between vimentin and CD133 expression (P = 0.020). CD133 was a stronger prognostic factor than an EMT marker. Elevated CD133 expression is the signature marker of EMT and CS association in lung adenocarcinoma. EMT and CS are associated in lung adenocarcinoma. Importantly, CD133 is suggested to be the key factor that links EMT and CS, thereby exacerbating tumor progression.

Published

2015

5. The role of growth differentiation factor 15 in the pathogenesis of primary myelofibrosis

Author

70605146, 90573676, 10252462, 80229286, Uchiyama, Tatsuki, Kawabata, Hiroshi, Miura, Yasuo, Yoshioka, Satoshi, Iwasa, Masaki, Yao, Hisayuki, Sakamoto, Soichiro, Fujimoto, Masakazu, Haga, Hironori, Kadowaki, Norimitsu, Maekawa, Taira, Takaori-Kondo, Akifumi, 70605146, 90573676, 10252462, 80229286, Uchiyama, Tatsuki, Kawabata, Hiroshi, Miura, Yasuo, Yoshioka, Satoshi, Iwasa, Masaki, Yao, Hisayuki, Sakamoto, Soichiro, Fujimoto, Masakazu, Haga, Hironori, Kadowaki, Norimitsu, Maekawa, Taira, and Takaori-Kondo, Akifumi

Published

2015