Updated on 2021/07/29

写真a

 
MATSUMURA Shigeru
 
Organization
Graduate School of Medicine Center for Research of Laboratory Animals and Medical Research Engineering Division Designated lecturer
Title
Designated lecturer

Degree 1

  1. 博士(生命科学) ( 2007.5   京都大学 ) 

 

Papers 7

  1. Oncolytic herpes simplex virus HF10 (canerpaturev) promotes accumulation of CD8(+)PD-1(-) tumor-infiltrating T cells in PD-L1-enriched tumor microenvironment

    Eissa Ibrahim Ragab, Mukoyama Nobuaki, Abdelmoneim Mohamed, Naoe Yoshinori, Matsumura Shigeru, Bustos-Villalobos Itzel, Ichinose Toru, Miyajima Noriyuki, Morimoto Daishi, Tanaka Maki, Fujimoto Yasushi, Sone Michihiko, Kodera Yasuhiro, Kasuya Hideki

    INTERNATIONAL JOURNAL OF CANCER   Vol. 149 ( 1 ) page: 214 - 227   2021.7

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    Language:Japanese   Publisher:International Journal of Cancer  

    Oncolytic viruses (OVs) remodel the tumor microenvironment by switching a “cold” tumor into a “hot” tumor with high CD8+ T-cell infiltration. CD8+ T-cell activity plays an essential role in the antitumor efficacy of OVs. However, the activity of T cells is impaired by the programmed cell death protein-1/programmed cell death-ligand 1 (PD-1/PD-L1) interaction. To date, it remains unclear why OVs alone have a significant antitumor activity even when PD-L1 expression persists on tumor or immune cells. In this study, we found that canerpaturev (C-REV) treatment significantly suppressed tumor growth, even though it induced a significant increase in PD-L1 expression in tumors in vivo as well as persistence of high PD-L1 expression on antigen-presenting cells (macrophage and dendritic cells [DCs]). Surprisingly, we observed that C-REV treatment increased the abundance of activated CD8+PD-1− tumor-infiltrating lymphocytes (TILs) in the tumor on both the injected and contralateral sides, although infiltration of CD8+PD-1high TILs into the tumor was observed in the control group. Moreover, the difference in PD-1 expression was observed only in tumors after treatment with C-REV, whereas most CD8+ T cells in the spleen, tumor-draining lymph nodes and blood were PD-1-negative, and this did not change after C-REV treatment. In addition, changes in expression of T-cell immunoglobulin and mucin-domain containing-3 and T-cell immune-receptor with Ig and ITIM domains were not observed on CD8+ TILs after C-REV treatment. Taken together, our findings may reveal mechanisms that allow OVs to trigger an antitumor immune response, irrespective of a PD-L1-enriched tumor microenvironment, by recruitment of CD8+PD-1− TILs.

    DOI: 10.1002/ijc.33550

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  2. C-REV Retains High Infectivity Regardless of the Expression Levels of cGAS and STING in Cultured Pancreatic Cancer Cells

    Morimoto Daishi, Matsumura Shigeru, Bustos-Villalobos Itzel, Sibal Patricia Angela, Ichinose Toru, Naoe Yoshinori, Eissa Ibrahim Ragab, Abdelmoneim Mohamed, Mukoyama Nobuaki, Miyajima Noriyuki, Tanaka Maki, Kodera Yasuhiro, Kasuya Hideki

    CELLS   Vol. 10 ( 6 )   2021.6

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  3. Combination of Cetuximab and Oncolytic Virus Canerpaturev Synergistically Inhibits Human Colorectal Cancer Growth

    Wu Zhiwen, Ichinose Toru, Naoe Yoshinori, Matsumura Shigeru, Villalobos Itzel Bustos, Eissa Ibrahim Ragab, Yamada Suguru, Miyajima Noriyuki, Morimoto Daishi, Mukoyama Nobuaki, Nishikawa Yoko, Koide Yusuke, Kodera Yasuhiro, Tanaka Maki, Kasuya Hideki

    MOLECULAR THERAPY-ONCOLYTICS   Vol. 13   page: 107 - 115   2019.6

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    Language:Japanese   Publisher:Molecular Therapy - Oncolytics  

    The naturally occurring oncolytic herpes simplex virus canerpaturev (C-REV), formerly HF10, proved its therapeutic efficacy and safety in multiple clinical trials against melanoma, pancreatic, breast, and head and neck cancers. Meanwhile, patients with colorectal cancer, which has increased in prevalence in recent decades, continue to have poor prognosis and morbidity. Combination therapy has better response rates than monotherapy. Hence, we investigated the antitumor efficacy of cetuximab, a widely used anti-epidermal growth factor receptor (EGFR) monoclonal antibody, and C-REV, either alone or in combination, in vitro and in an in vivo human colorectal xenograft model. In human colorectal cancer cell lines with different levels of EGFR expression (HT-29, WiDr, and CW2), C-REV exhibited cytotoxic effects in a time- and dose-dependent manner, irrespective of EGFR expression. Moreover, cetuximab had no effect on viral replication in vitro. Combining cetuximab and C-REV induced a synergistic antitumor effect in HT-29 tumor xenograft models by promoting the distribution of C-REV throughout the tumor and suppressing angiogenesis. Application of cetuximab prior to C-REV yielded better tumor regression than administration of the drug after the virus. Thus, cetuximab represents an ideal virus-associated agent for antitumor therapy, and combination therapy represents a promising antitumor strategy for human colorectal cancer.

    DOI: 10.1016/j.omto.2019.04.004

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  4. STING is dispensable for low susceptibility for HF10 in pancreatic cell lines

    Matsumura Shigeru, Morimoto Daishi, Noe Yoshinori, Ichinose Toru, Tanaka Maki, Kodera Yasuhiro, Kasuya Hideki

    CANCER SCIENCE   Vol. 109   page: 1328 - 1328   2018.12

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    Language:Japanese  

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  5. The Current Status and Future Prospects of Oncolytic Viruses in Clinical Trials against Melanoma, Glioma, Pancreatic, and Breast Cancers

    Eissa Ibrahim Ragab, Bustos-Villalobos Itzel, Ichinose Toru, Matsumura Shigeru, Naoe Yoshinori, Miyajima Noriyuki, Morimoto Daishi, Mukoyama Nobuaki, Wu Zhiwen, Tanaka Maki, Hasegawa Hitoki, Sumigama Seiji, Aleksic Branko, Kodera Yasuhiro, Kasuya Hideki

    CANCERS   Vol. 10 ( 10 )   2018.10

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    Language:Japanese   Publisher:Cancers  

    Oncolytic viral therapy has been accepted as a standard immunotherapy since talimogene laherparepvec (T-VEC, Imlygic®) was approved by the Food and Drug Administration (FDA) and European Medicines Agency (EMA) for melanoma treatment in 2015. Various oncolytic viruses (OVs), such as HF10 (Canerpaturev—C-REV) and CVA21 (CAVATAK), are now actively being developed in phase II as monotherapies, or in combination with immune checkpoint inhibitors against melanoma. Moreover, in glioma, several OVs have clearly demonstrated both safety and a promising efficacy in the phase I clinical trials. Additionally, the safety of several OVs, such as pelareorep (Reolysin®), proved their safety and efficacy in combination with paclitaxel in breast cancer patients, but the outcomes of OVs as monotherapy against breast cancer have not provided a clear therapeutic strategy for OVs. The clinical trials of OVs against pancreatic cancer have not yet demonstrated efficacy as either monotherapy or as part of combination therapy. However, there are several oncolytic viruses that have successfully proved their efficacy in different preclinical models. In this review, we mainly focused on the oncolytic viruses that transitioned into clinical trials against melanoma, glioma, pancreatic, and breast cancers. Hence, we described the current status and future prospects of OVs clinical trials against melanoma, glioma, pancreatic, and breast cancers.

    DOI: 10.3390/cancers10100356

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  6. Tbx3-dependent amplifying stem cell progeny drives interfollicular epidermal expansion during pregnancy and regeneration.

    Ichijo R, Kobayashi H, Yoneda S, Iizuka Y, Kubo H, Matsumura S, Kitano S, Miyachi H, Honda T, Toyoshima F

    Nature communications   Vol. 8 ( 1 ) page: 508   2017.9

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    Language:English  

    DOI: 10.1038/s41467-017-00433-7

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  7. Katanin p80, NuMA and cytoplasmic dynein cooperate to control microtubule dynamics

    Jin Mingyue, Pomp Oz, Shinoda Tomoyasu, Toba Shiori, Torisawa Takayuki, Furuta Ken'ya, Oiwa Kazuhiro, Yasunaga Takuo, Kitagawa Daiju, Matsumura Shigeru, Miyata Takaki, Tan Thong Teck, Reversade Bruno, Hirotsune Shinji

    SCIENTIFIC REPORTS   Vol. 7   page: 39902   2017.1

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    Language:Japanese   Publisher:Scientific Reports  

    Human mutations in KATNB1 (p80) cause severe congenital cortical malformations, which encompass the clinical features of both microcephaly and lissencephaly. Although p80 plays critical roles during brain development, the underlying mechanisms remain predominately unknown. Here, we demonstrate that p80 regulates microtubule (MT) remodeling in combination with NuMA (nuclear mitotic apparatus protein) and cytoplasmic dynein. We show that p80 shuttles between the nucleus and spindle pole in synchrony with the cell cycle. Interestingly, this striking feature is shared with NuMA. Importantly, p80 is essential for aster formation and maintenance in vitro. siRNA-mediated depletion of p80 and/or NuMA induced abnormal mitotic phenotypes in cultured mouse embryonic fibroblasts and aberrant neurogenesis and neuronal migration in the mouse embryonic brain. Importantly, these results were confirmed in p80-mutant harboring patient-derived induced pluripotent stem cells and brain organoids. Taken together, our findings provide valuable insights into the pathogenesis of severe microlissencephaly, in which p80 and NuMA delineate a common pathway for neurogenesis and neuronal migration via MT organization at the centrosome/spindle pole.

    DOI: 10.1038/srep39902

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KAKENHI (Grants-in-Aid for Scientific Research) 2

  1. 癌を支える癌関連間葉系幹細胞の癌ワクチンへの標的化

    Grant number:18H02691  2018.4 - 2022.3

    松村 繁

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    Authorship:Principal investigator 

    Grant amount:\17160000 ( Direct Cost: \13200000 、 Indirect Cost:\3960000 )

    ウイルス改変のためのターゲットベクターの作成を終え改変ウイルス作製過程へと進んでいる。改変ウイルス作製は2段階に分けられ、現在第一段階:ゲートウェイシステムを組み込んだウイルス作製を進めている。組み換え用に必要なコンストラクトの作成を並行して行っている。引き続きウイルス作製を遂行していく予定である。ただし、ウイルス作製にあたっては、vero細胞およびCrisprCas9システムを用いているが、ウイルスゲノム、ターゲットベクター、CrisprCas9-guideRNAベクターのコトランスフェクション効率に依存し、ウイルスゲノム組み換え効率が低い場合には、細胞やトランスフェクション試薬等の再条件検討が必要となる可能性を含む。
    間葉系幹細胞の単離培養は、培養可能な血清検討を経て、ようやく確立することができた。間葉系幹細胞と乳癌細胞の共培養でのマウスへの接種では、間葉系幹細胞を共培養した際にマウスが短命であった。まだ実験条件の詳細な検討が必要な段階である。ようやく腫瘍形成をさせられるようになった段階であり、結果の解析および結論を得るには更なる実験が必要である。またこの時、肺転移は見られなかった。引き続き条件検討も行う。
    間葉系幹細胞へのレンチウイルスを用いた遺伝子導入もレンチウイルス作製段階にある。iCaspaseの系に変えてジフテリア毒素とジフテリア毒素受容体(HBEGF)による選択的殺細胞の系確立を進めている。これにより、間葉系幹細胞を選択的に殺す系の確立を目指すとともに、腫瘍溶解性ウイルスとの比較を行っていく予定である。
    癌細胞の癌幹細胞を蛍光ラベルするための系であるが、当初のプロモーターに疑義が生じたため、ALDHプロモーターを用いたコンストラクトへ計画を変更しそれもようやく80%を終えた。次年度にこのプロモーターで癌幹細胞がラベルできるのかを検証するため、細胞株樹立を行い、その性質をin vitroおよびin vivoにて検証する予定である。
    いまだ準備段階である。ウイルス改変は、まだ作成段階にある。ようやく実験系の各条件が整ってきた感じである。着実に研究は進んでおり、次年度は準備を整え、結果を検証する実験をできるものと考えられる。残りの期間で、当初の目標地点へ到達できるよう研究を加速していくつもりである。
    ここまで進めたものを、ひとつひとつ確かめながら着実に進めていく予定である。ウイルス改変とマウス実験、癌幹細胞と必要な各実験材料を確実に準備して目標とする実験を次年度行う予定である。

  2. Spindle orientation control via caveolin1 and Ak2 in skin development

    Grant number:15K09741  2015.4 - 2018.3

    Matsumura Shigeru

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    Authorship:Principal investigator 

    Grant amount:\4810000 ( Direct Cost: \3700000 、 Indirect Cost:\1110000 )

    It has been reported that spindle orientation control in skin basal cells has a pivotal role in skin development. Caveolin1, Ak2 and Pank2 are candidates, involved in spindle orientation control by our screen in adherent cultured cells. We hypothesized that these genes have a role in a common spindle orientation regulatory pathway, especially in metabolic pathway in sugar and lipids. However, although the inhibition of metabolic pathway resulted in spindle disregulation, we could not find a common pathway behind three candidate genes. We found that spindle misorientation in skin basal cells during embryonic skin development in caveolin1 ko mice. But we could not obtained Ak2 floxed homo mice at last and could not obtain any results if Ak2 regulates spindle orientation in skin development. To elucidate further insights, studies on more detailed analysis in metabolisms should be required.