GEN-0101(GEN-0101) - 在研适应症：间皮瘤，前列腺癌_专利_临床

概要

基本信息

药物类型

溶瘤病毒

别名

HVJ-E、GEN 0101、GEN0101

+ [1]

靶点-

作用方式

刺激剂

作用机制

免疫刺激剂

治疗领域

在研适应症

非在研适应症

原研机构

在研机构

ISHIHARA SANGYO KAISHA Ltd.

非在研机构

TSD Japan, Inc.

权益机构-

最高研发阶段临床2期

首次获批日期-

最高研发阶段(中国)-

特殊审评-

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关联

9

项与 GEN-0101 相关的临床试验

NCT03818893

/ Unknown status临床2期IIT

Phase Ib/II Investigator Initiated Safety and Efficacy Clinical Trial of Combination Therapy of Intracutaneous GEN0101 With Intravenous Pembrolizmub in Patients Who Have Advanced Melanoma

This is a multi-center, open-labeled, non-randomized, single arm investigator-initiated trial to evaluate the safety and efficacy of GEN0101 and Pembrolizmub combination in patients with advanced melanoma.

开始日期2019-03-01

申办/合作机构

Osaka University

[+2]

JPRN-jRCT2080224548

/ Completed临床2期IIT

Phase II multicenter investigator-initiated clinical trial to evaluate safety and efficacy of combination therapy with GEN0101 and standard chemotherapy in patients suffering from pleural mesothelioma.

开始日期2019-01-10

申办/合作机构-

JPRN-jRCTc051190054

/ Completed临床1期IIT

Open-label clinical study for safety and preliminary efficacy of HiDCV-OS1 Hybrid cell (dendritic and tumor fusion cells) and subsequent subcutaneous administration of GEN0101 in patients with recalcitrant residual or relapsed ovarian cancer after strict chemotherapy. - HiDCV-OS1

开始日期2018-05-30

申办/合作机构-

100 项与 GEN-0101 相关的临床结果

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100 项与 GEN-0101 相关的转化医学

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100 项与 GEN-0101 相关的专利（医药）

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71

项与 GEN-0101 相关的文献（医药）

2025-06-01·Journal for ImmunoTherapy of Cancer

HVJ-E links Apolipoprotein d to antitumor effects

Article

作者: Kimura, Tadashi ; Ino, Yoko ; Ohta, Noriko ; Sawada, Kenjiro ; Hisatomi, Yuuta ; Kitamura, Koji ; Yusa, Kosuke ; Inubushi, Satoko ; Saga, Kotaro ; Ohashi, Riuko ; Takahashi, Hidehisa ; Nimura, Keisuke ; Fukino, Katsuya ; Yoshimura, Yasuhide ; Ishibashi, Airi ; Suzuki, Hidefumi ; Uegaki, Yuko ; Tanemura, Atsushi ; Kimura, Yayoi ; Kaneda, Yasufumi ; Kiyohara, Eiji ; Ishida, Kyoso

Background:

Virotherapy eradicates tumors by directly killing cancer cells and causing adjuvant effects. However, the mechanism by which non-replicating virotherapy exerts anti-tumor effects is unclear.

Methods:

In this study, we investigated the genes that mediate the anti-tumor effects of ultraviolet (UV)-irradiated Hemagglutinating Virus of Japan envelope (HVJ-E) using RNA sequencing, gene knockout, and a drug-inducible gene expression system. We examined the antitumor effects of Apolipoprotein d (Apod) using genome-wide CRISPR library screening, in situ biotinylation combined with mass spectrometry, flow cytometry, biochemistry, and tumor-bearing mouse models.

Results:

Here, we show that HVJ-E represses tumor growth via Irf7-induced Apod expression in tumor cellsin vivo. Irf7 in B16F10 cells is a pivotal transcription factor for HVJ-E-induced anti-tumor effects. Apod substantially suppresses tumor growth even in HVJ-E-insensitive tumors. Apod is required to increase NKG2D-ligand genes in HVJ-E-treated tumors. Genome-wide CRISPR library screening andin situbiotinylation of Apod reveal an association of Apod with ERK2. Mechanistically, Apod prevents the nuclear translocation of ERK2 and Importin7, increasing NKG2D-ligands expression in B16F10 cells and attenuating tumor growth. Treating a local tumor with a combination therapy of Apod with the anti-OX40, T cell costimulatory molecule, antibody substantially repressed tumor growth in target and non-target lesions alongside T cell activation.

Conclusion:

Our findings provide insights into the molecular mechanisms of how HVJ-E induces anti-tumor effects and can aid the development of therapeutic strategies for eliciting anti-tumor immunity.

2024-12-01·Molecular Therapy: Oncology

Local treatment of HVJ-E with T cell costimulatory molecule stimulation elicits systemic anti-tumor effects

Article

作者: Ohta, Noriko ; Yagita, Hideo ; Hisatomi, Yuuta ; Inubushi, Satoko ; Hashimoto, Shinichi ; Li, Yue ; Kaneda, Yasufumi ; Kiyohara, Eiji ; Kitamura, Koji ; Ohashi, Riuko ; Ishibashi, Airi ; Uegaki, Yuko ; Yoshimura, Yasuhide ; Saga, Kotaro ; Tanemura, Atsushi ; Nimura, Keisuke ; Iwabuchi, Sadahiro ; Ishida, Kyoso

The tumor-infiltrating lymphocyte (TIL) is a crucial factor in controlling tumor growth. A therapeutic method activating TIL is desired for treating patients with metastatic tumors. Here, we show that treating a local tumor with a combination therapy of UV-irradiated hemagglutinating virus of Japan envelope (HVJ-E) plus agonist antibodies, including OX40, against T cell costimulatory molecules induces systemic anti-tumor effects in a T cell-dependent manner in multiple cancer cell lines. Transcriptome and T cell receptor repertoire analyses revealed that HVJ-E + anti-OX40 antibody treatment activates CD4 and CD8 T cells and promotes T cell trafficking between tumors. These systemic anti-tumor effects required an association between Nkg2d and Nkg2d ligands. Our findings provide insights into how systemic anti-tumor effects are induced and may help the development of therapeutic strategies for eliciting such effects.

2024-01-12·Reproduction (Cambridge, England)

The press-assisted fusion scheme significantly mitigates the quantity of HVJ-E required in mitochondrial replacement techniques

Article

作者: Lin, Kaibo ; Li, Wenzhi ; Kuang, Yanping ; Chen, Chen ; Lyu, Qifeng ; Ma, Meng ; Jin, Wei ; Liao, Xiaoyu ; Jiang, Shutian ; Li, Danjun

In brief:

The impact of HVJ-E employed in mitochondrial replacement techniques (MRTs) on embryonic development remains uncertain. This study has exhibited the influence of HVJ-E utilized in MRTs on embryonic development and has devised a novel HVJ-E-induced fusion approach to curtail the amount of HVJ-E employed in MRTs.

Abstract:

Mitochondrial replacement techniques (MRTs) provide a viable option for women carrying pathogenic mitochondrial DNA (mtDNA) variants to conceive disease-free offspring with a genetic connection. In comparison to electrofusion, HVJ-E-induced fusion has been identified as the most promising approach for clinical translation of MRTs due to its absence of electrical interference. However, despite confirmation of the absence of RNA activity in HVJ-E, a reduction in blastocyst quality has been observed in various MRTs studies utilizing the HVJ-E-induced fusion scheme. Recent investigations have revealed a dose-dependent elevation of reactive oxygen species (ROS) levels in various cancer cells incubated with HVJ-E. However, the impact of HVJ-E as a sole determinant on embryonic development in MRTs remains unverified. This investigation establishes that the augmented concentration of HVJ-E utilized in the conventional HVJ-E fusion protocol is an autonomous variable that influences embryonic development in MRTs. This effect may be attributed to amplified DNA damage resulting from heightened levels of ROS in reconstructed embryos. To mitigate the presence of HVJ-E in reconstructed zygotes while maintaining optimal fusion efficiency in MRTs, a novel HVJ-E-induced fusion approach was devised, namely, press-assisted fusion. This technique offers potential advantages in reducing detrimental factors that impede embryo development in MRTs.

100 项与 GEN-0101 相关的药物交易

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研发状态

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适应症	最高研发状态	国家/地区	公司	日期
局部晚期黑色素瘤	临床2期	日本	ISHIHARA SANGYO KAISHA Ltd.	2019-03-01
局部晚期黑色素瘤	临床2期	日本	Osaka University	2019-03-01
间皮瘤	临床2期	-	ISHIHARA SANGYO KAISHA Ltd.	-
间皮瘤	临床2期	-	Osaka University	-
间皮瘤	临床2期	-	TSD Japan, Inc.	-
前列腺癌	临床2期	-	ISHIHARA SANGYO KAISHA Ltd.	-
前列腺癌	临床2期	-	Osaka University	-
前列腺癌	临床2期	-	TSD Japan, Inc.	-
去势抵抗性前列腺癌	临床1期	日本	Osaka University	2015-05-01

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临床结果

适应症

分期

评价

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研究	分期	人群特征	评价人数	分组	结果	评价	发布日期


WCLC2018	N/A	恶性胸膜间皮瘤	6	HVJ-E	製遞觸顧構齋膚鏇窪鬱(網襯醖簾餘顧蓋鹹壓範) = 83.3% 構醖壓衊廠艱顧膚顧鑰 (製襯獵獵獵淵糧壓鹹繭 ) 更多	-	2018-09-24