更新于：2024-09-19

TNFRSF21

更新于：2024-09-19

基本信息

别名

CD358、Death receptor 6、DR6

+ [4]

简介

Promotes apoptosis, possibly via a pathway that involves the activation of NF-kappa-B. Can also promote apoptosis mediated by BAX and by the release of cytochrome c from the mitochondria into the cytoplasm. Plays a role in neuronal apoptosis, including apoptosis in response to amyloid peptides derived from APP, and is required for both normal cell body death and axonal pruning. Trophic-factor deprivation triggers the cleavage of surface APP by beta-secretase to release sAPP-beta which is further cleaved to release an N-terminal fragment of APP (N-APP). N-APP binds TNFRSF21; this triggers caspase activation and degeneration of both neuronal cell bodies (via caspase-3) and axons (via caspase-6). Negatively regulates oligodendrocyte survival, maturation and myelination. Plays a role in signaling cascades triggered by stimulation of T-cell receptors, in the adaptive immune response and in the regulation of T-cell differentiation and proliferation. Negatively regulates T-cell responses and the release of cytokines such as IL4, IL5, IL10, IL13 and IFNG by Th2 cells. Negatively regulates the production of IgG, IgM and IgM in response to antigens. May inhibit the activation of JNK in response to T-cell stimulation.

关联

项与 TNFRSF21 相关的药物

Angiocidin (Protheragen)

靶点

TNFRSF21

作用机制

TNFRSF21拮抗剂 [+1]

在研机构

Protheragen, Inc.

原研机构

Protheragen, Inc.

在研适应症

急性髓性白血病

非在研适应症-

最高研发阶段临床前

首次获批国家/地区-

首次获批日期1800-01-20

HG-1334

靶点

TNFRSF21

作用机制

TNFRSF21 modulators

在研机构-

原研机构

Human Genome Sciences, Inc.

在研适应症-

非在研适应症-

最高研发阶段无进展

首次获批国家/地区-

首次获批日期1800-01-20

HG-1309

靶点

TNFRSF21

作用机制

TNFRSF21 modulators

在研机构-

原研机构

Human Genome Sciences, Inc.

在研适应症-

非在研适应症

免疫系统疾病

最高研发阶段无进展

首次获批国家/地区-

首次获批日期1800-01-20

100 项与 TNFRSF21 相关的临床结果

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100 项与 TNFRSF21 相关的转化医学

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0 项与 TNFRSF21 相关的专利（医药）

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487

项与 TNFRSF21 相关的文献（医药）

2024-12-31·OncoImmunology

Cerebrospinal fluid immunological cytokines predict intracranial tumor response to immunotherapy in non-small cell lung cancer patients with brain metastases

Article

作者: Hou, Xue ; Li, Meichen ; Chen, Likun ; Jiang, Honghua ; Yu, Hui ; Chen, Jing ; Xie, Dan ; Zhang, Baishen

BackgroundImmunotherapy has shown intracranial efficacy in non-small cell lung cancer (NSCLC) patients with brain metastases. However, predictive biomarkers for intracranial response to immunotherapy are lacking. This post-hoc analysis aimed to explore the potential of immunological cytokines in cerebrospinal fluid (CSF) to predict intracranial tumor response to immunotherapy in patients with brain metastases.MethodsTreatment-naive NSCLC patients with brain metastases who received camrelizumab plus chemotherapy were enrolled. Paired plasma and CSF samples were prospectively collected at baseline and the first treatment assessment. All samples were analyzed for 92 immuno-oncology cytokines using Olink's panels.ResultsA total of 28 patients were included in this analysis. At baseline, most immunological cytokines were significantly lower in CSF than in plasma, whereas a subset comprising CD83, PTN, TNFRSF21, TWEAK, ICOSLG, DCN, IL-8, and MCP-1, was increased in CSF. Baseline CSF levels of LAMP3 were significantly higher in patients with intracranial tumor response, while the levels of CXCL10, IL-12, CXCL11, IL-18, TIE2, HGF, and PDCD1 were significantly lower. Furthermore, the CXCL10, CXCL11, TIE2, PDCD1, IL-18, HGF, and LAMP3 in CSF were also significantly associated with intracranial progression-free survival for immunotherapy. The identified cytokines in CSF were decreased at the first treatment evaluation in patients with intracranial tumor response. The logistic CSF immuno-cytokine model yielded an AUC of 0.91, as compared to PD-L1 expression (AUC of 0.72).ConclusionsImmunological cytokines in CSF could predict intracranial tumor response to immunotherapy in NSCLC patients with brain metastases, and the findings warrant validation in a larger prospective cohort study.Trial registrationClinicalTrials.gov identifier: NCT04211090.

2024-07-01·Genes & Genomics

eEF1A1 regulates the expression and alternative splicing of genes associated with Parkinson’s disease in U251 cells

Article

作者: Zhang, Yan ; Aimaier, Guliqiemu ; Ma, Jianhua ; Lei, Jing ; Aisha, Zaolaguli

BACKGROUNDEukaryotic elongation factor 1A1 (eEF1A1) is an RNA-binding protein that is associated with PARK2 activity in cells, suggesting a possible role in Parkinson's disease (PD).OBJECTIVETo clear whether eEF1A1 plays a role in PD through transcriptional or posttranscriptional regulation.METHODSThe GSE68719 dataset was downloaded from the GEO database, and the RNA-seq data of all brain tissue autopsies were obtained from 29 PD patients and 44 neurologically normal control subjects. To inhibit eEF1A1 from being expressed in U251 cells, siRNA was transfected into those cells, and RNA-seq high-throughput sequencing was used to determine the differentially expressed genes (DEGs) and differentially alternative splicing events (ASEs) resulting from eEF1A1 knockdown.RESULTSeEF1A1 was significantly overexpressed in PD brain tissue in the BA9 area. GO and KEGG enrichment analyses revealed that eEF1A1 knockdown significantly upregulated the expression of the genes CXCL10, NGF, PTX3, IL6, ST6GALNAC3, NUPR1, TNFRSF21, and CXCL2 and upregulated the alternative splicing of the genes ACOT7, DDX10, SHMT2, MYEF2, and NDUFAF5. These genes were enriched in pathways related to PD pathogenesis, such as apoptosis, inflammatory response, and mitochondrial dysfunction.CONCLUSIONThe results suggesting that eEF1A1 involved in the development of PD by regulating the differential expression and alternative splicing of genes, providing a theoretical basis for subsequent research.

2024-05-27·British Journal of Cancer

The prognostic value of MEK pathway–associated estrogen receptor signaling activity for female cancers

Article

作者: Wong, Kwong-Kwok ; Gershenson, David M ; Ng, Chun Wai ; Tsang, Yvonne T M

AbstractBackgroundOther than for breast cancer, endocrine therapy has not been highly effective for gynecologic cancers. Endocrine therapy resistance in estrogen receptor positive gynecologic cancers is still poorly understood. In this retrospective study, we examined the estrogen receptor (ER) signaling pathway activities of breast, ovarian, endometrial, and cervical cancers to identify those that may predict endocrine therapy responsiveness.MethodsClinical and genomic data of women with breast and gynecological cancers were downloaded from cBioPortal for Cancer Genomics. Estrogen receptor alpha (ESR1) expression level and sample-level pathway enrichment scores (EERES) were calculated to classify patients into four groups (low/high ESR1 and low/high EERES). Correlation between ESR1/EERES score and survival was further validated with RNAseq data from low-grade serous ovarian cancer. Pathway analyses were performed among different ESR1/EERES groups to identify genes that correlate with endocrine resistance, which are validated using Cancer Cell Line Encyclopedia gene expression and Genomics of Drug Sensitivity in Cancer data.ResultsWe identified a novel combined prognostic value of ESR1 expression and the corresponding estrogen response signaling (EERES score) for breast cancer. The combined prognostic value (ESR1/EERES) may be applicable to other gynecologic cancers. More importantly, we discovered that ER signaling can cross-regulate MEK pathway activation. We identified downstream genes in the MEK pathway (EPHA2, INAVA, MALL, MPZL2, PCDH1, and TNFRSF21) that are potential endocrine therapy response biomarkers.ConclusionThis study demonstrated that targeting both the ER and the ER signaling activity related MEK pathway may aid the development of endocrine therapy strategies for personalized medicine.

项与 TNFRSF21 相关的新闻（医药）

2024-08-03

·生物谷

细胞治疗前沿探索！Nat. Cell Biol | 厦门大学吴乔课题组发现全长GSDME通过非剪切方式诱导细胞焦亡

细胞焦亡（Pyroptosis）是由Gasdermin（GSDM）家族蛋白介导的程序性细胞坏死。近年来，大量的研究表明细胞焦亡与多种疾病相关，包括败血症、细菌感染、慢性炎症、自身免疫病、神经退行性疾病以及肿瘤等。前期研究表明，GSDM蛋白的C端对N端的抑制作用使得全长Gasdermin蛋白处于自抑制状态，阻碍其诱导细胞焦亡。因此，在细胞焦亡过程中，Gasdermin蛋白需要被蛋白酶剪切释放其具备打孔活性的N端结构域，再转运至细胞膜形成孔道，导致细胞膜通透性改变，细胞不断吸水胀大，最终引起细胞焦亡。前期，吴乔课题组在细胞焦亡领域取得了多项研究成果，包括阐明了Tom20感知铁激活的ROS信号促进细胞焦亡抑制黑色素瘤生长的机制（Cell Research，2018，封面文章）；揭示了代谢产物α-KG通过死亡受体DR6激活caspase-8诱导GSDMC依赖的细胞焦亡机制（Cell Research，2021，highlighted in the cover）；发现甘露糖可以通过激活 AMPK，磷酸化GSDME的第6位苏氨酸，阻断caspase-3剪切GSDME，进而抑制细胞焦亡。这一新发现进一步应用于临床，证实了甘露糖可以减轻化疗药物引起的正常组织焦亡所导致的毒副作用（Cell Research，2023，封面文章）。系列研究成果丰富了细胞焦亡的调控网络，为细胞焦亡的临床应用提供了理论依据。在细胞应激状态下，全长Gasdermin能否直接诱导细胞焦亡以及如何解除自抑制状态并不清楚。邵峰院士课题组早期发现在GSDM-C端和GSDM-N端结合的界面引入氨基酸突变，可以解除Gasdermin的自抑制状态，全长Gasdermin则具备了自主诱导细胞焦亡的能力，首次提示Gasdermin蛋白可以通过不依赖于蛋白酶剪切的方式诱导细胞焦亡（Nature，2016）。近期，美国吴皓院士课题组在Nature发文，报道了ROS通过诱导全长GSDMD发生棕榈酰化修饰，使其具备了成孔和诱导细胞焦亡的能力（Nature, 2024）。与此同时，邵峰院士团队也在Science 发表文章，揭示了在低等真核生物中两类只含有膜打孔结构域的GSDM蛋白可以分别通过氧化还原调控或配对的分子间相互作用释放其膜打孔活性，从而诱导焦亡（Science, 2024）。这两篇文章进一步证明全长Gasdermin蛋白（如GSDMD）可以通过不依赖于蛋白酶剪切的方式诱导细胞焦亡。 2024年7月12日，吴乔课题组在Nature Cell Biology在线发表文章"Fulllength GSDME mediates pyroptosis independent from cleavage"，从机制上阐释了全长GSDME通过剪切非依赖的方式诱导细胞焦亡的新通路。研究发现，当细胞被UVC照射后，线粒体发生断裂（mitochondrial fission），导致线粒体ROS（mitoROS）提高，进而触发细胞色素c的过氧化物酶活性，氧化线粒体心磷脂，促进lipid ROS的产生。 Lipid ROS信号被GSDME直接感知，导致GSDME氧化多聚。与此同时，UVC照射导致的DNA损伤激活PARP1产生大量的PAR（Poly(ADP-ribose)）并释放到胞浆，胞浆中的PAR则与PARP5结合，激活 PARP5活性，以此促进其与GSDME结合，诱导GSDME发生PARylation修饰，导致GSDME构象发生改变，解除GSDME-C端对其N端的自抑制状态，进而促进GSDME感知lipid-ROS信号。这两种不同的蛋白修饰协同作用导致了全长GSDME靶向质膜定位并打孔，从而诱导细胞焦亡。基于这一新发现，作者进一步确定了全长GSDME介导的细胞焦亡不仅仅局限于UVC照射。同时激活PARP的活性和提高lipid ROS水平的药物或者DNA损伤诱导剂和lipid ROS诱导剂联合处理同样能够诱导全长 GSDME 依赖的细胞焦亡。该研究挑战了焦亡诱导需要蛋白酶剪切的传统概念，阐明了全长GSDME不依赖蛋白酶剪切诱导细胞焦亡的新机制及其调控模式，进一步证实了全长GSDME与GSDMD一样可以直接诱导细胞焦亡，为研究细胞焦亡的新范式奠定了理论基础。全长GSDME通过非剪切方式诱导细胞焦亡的信号网络和调控机制模式图生命科学学院吴乔教授和陈航姿教授为论文的共同通讯作者，博士后周波、博士生江志洪和硕士生戴梦燃为论文的共同第一作者。文章链接： https://www.nature.com/articles/s41556-024-01463-2 原文链接： https://life.xmu.edu.cn/info/1045/27831.htm 本文仅用于学术分享，转载请注明出处。若有侵权，请联系微信：bioonSir 删除或修改！

细胞疗法临床研究

2024-08-02

·生物探索

Nat Cell Biol | 吴乔/陈航姿合作揭示全长GSDME通过剪切非依赖的方式诱导细胞焦亡

引言细胞焦亡 (Pyroptosis) 是由Gasdermin（GSDM）家族蛋白介导的程序性细胞坏死。GSDM蛋白的C端对N端的抑制作用使得全长Gasdermin蛋白处于自抑制状态，阻碍其诱导细胞焦亡。因此，既往研究都认为在细胞焦亡过程中，Gasdermin蛋白需要被蛋白酶剪切释放其具备打孔活性的N端结构域，再转运至细胞膜打孔，导致细胞膜通透性改变，细胞不断吸水胀大，最终引起细胞焦亡。全长Gasdermin能否直接诱导细胞焦亡并不清楚。邵峰课题组早期发现在GSDM-C端和GSDM-N端结合的界面引入氨基酸突变，可以解除Gasdermin的自抑制状态，全长Gasdermin则具备了自主诱导细胞焦亡的能力，首次提示Gasdermin蛋白可以通过不依赖于蛋白酶剪切的方式诱导细胞焦亡（Nature, 2016）。近期，哈佛大学吴皓课题组在Nature发文，报道了ROS通过诱导全长GSDMD发生棕榈酰化修饰，使其具备了成孔和诱导细胞焦亡的能力（Nature, 2024）。与此同时，邵峰团队也在Science发表文章，揭示了在低等真核生物中两类只含有膜打孔结构域的GSDM蛋白可以分别通过氧化还原调控或配对的分子间相互作用释放其膜打孔活性，从而诱导焦亡（Science, 2024，Science丨丁璟珒/邵峰合作揭示真核生物焦亡蛋白GSDM非酶切依赖的全新激活机制）。这两篇文章证明了全长Gasdermin蛋白（如GSDMD）可以通过不依赖于蛋白酶剪切的方式诱导细胞焦亡。 2024年7月31日，吴皓教授受邀在Nature Cell Biology杂志的News & Views专栏撰写题为Cleavage-independent GSDME activation by UVC的亮点文章，介绍厦大生科院吴乔教授和陈航姿教授合作在细胞焦亡研究领域取得的最新重要进展。吴皓教授通过长篇幅系统总结了该研究的创新发现。当细胞被高强度的UVC照射后，线粒体发生断裂（mitochondrial fission），导致线粒体ROS（mito-ROS）提高，进而触发细胞色素c的过氧化物酶活性，氧化线粒体心磷脂，促进lipid ROS的产生。Lipid ROS信号被GSDME直接感知，导致GSDME氧化多聚。与此同时，UVC照射导致的DNA损伤激活PARP1产生大量的PAR（Poly(ADP-ribose)）并释放到胞浆，胞浆中的PAR则与PARP5结合，激活PARP5活性，以此促进其与GSDME结合，诱导GSDME发生PARylation修饰，导致GSDME构象发生改变，解除GSDME-C端对其N端的自抑制状态，进而促进GSDME感知lipid-ROS信号。这两种不同的蛋白修饰协同作用导致了全长GSDME靶向质膜定位并打孔，从而诱导细胞焦亡。基于这一新发现，作者进一步确定了全长GSDME介导的细胞焦亡不仅仅局限于UVC照射。同时激活PARP的活性和提高lipid ROS水平的药物或者DNA损伤诱导剂和lipid ROS诱导剂联合处理同样能够诱导全长GSDME依赖的细胞焦亡。最后，吴皓教授总结指出该项研究揭示了全长GSDME通过非经典的方式诱导细胞焦亡的新机制，不仅增强了对GSDMs如何非典型激活的见解，而且可能会启发研究者发现更多促进甚至抑制细胞死亡的生理靶标。同时，吴皓教授在文中还指出几个值得进一步探究的方向，包括：鉴于GSDME结构模型预测发生氧化修饰的半胱氨酸残基（Cys156/Cys180）之间的分子间距离太远，不利于二硫键的形成，需要通过GSDME结构分析进一步阐明GSDME中分子间二硫键是如何形成的；其他信号机制是否可以通过其他形式的蛋白修饰而汇聚到这条通路；此外，该通路如何与其他类型的细胞死亡和宿主免疫防御发生交互调控仍是一个悬而未决的问题；该通路在其他gasdermin蛋白、细胞类型和生物体中的有效性也需进一步探究。吴皓教授绘制的全长GSDME通过剪切非依赖的方式诱导细胞焦亡的模式图（Credit: Nature Cell Biology）据悉，该研究成果已于2024年7月12以Full-length GSDME mediates pyroptosis independent from cleavage 为题发表在Nature Cell Biology。吴乔课题组在细胞焦亡领域取得了多项研究成果，包括阐明了Tom20感知铁激活的ROS信号促进细胞焦亡抑制黑色素瘤生长的机制 (Cell Research，2018，封面文章)；揭示了代谢产物α-KG通过死亡受体DR6激活caspase-8诱导GSDMC依赖的细胞焦亡机制 (Cell Research，2021，highlighted in the cover)；发现甘露糖可以通过激活AMPK，磷酸化GSDME的第6位苏氨酸，阻断caspase-3剪切GSDME，进而抑制细胞焦亡。这一新发现进一步应用于临床，证实了甘露糖可以减轻化疗药物引起的正常组织焦亡所导致的毒副作用 (Cell Research，2023，封面文章)。系列研究成果丰富了细胞焦亡的调控网络，为细胞焦亡的临床应用提供了理论依据。近日他们在Nature Cell Biology在线发表文章，从机制上阐释了全长GSDME通过剪切非依赖的方式诱导细胞焦亡的新通路。该研究阐明了全长GSDME不依赖蛋白酶剪切诱导细胞焦亡的新机制及其调控模式，进一步证实了全长GSDME与GSDMD一样可以直接诱导细胞焦亡，为研究细胞焦亡的新范式奠定了理论基础。参考文献 https://www.nature.com/articles/s41556-024-01463-2 https://www. nature.com/articles/s41556-024-01470-3 责编|探索君排版|探索君文章来源|“BioArt” End 往期精选围观一文读透细胞死亡(Cell Death) | 24年Cell重磅综述（长文收藏版）热文 Cell | 是什么决定了细胞的大小？热文 Nature | 2024年值得关注的七项技术热文 Nature | 自身免疫性疾病能被治愈吗？科学家们终于看到了希望热文 CRISPR技术进化史 | 24年Cell综述

临床终止

2023-04-07

·FierceBiotech

Genentech probe of Marc Tessier-Lavigne paper finds no fraud evidence, but image 'anomalies' stay unresolved

A review did uncover a complaint “alleging scientific misconduct by another postdoc." Genentech has published the findings of its investigation into an alleged fraud and cover-up involving a 2009 Nature paper co-authored by Marc Tessier-Lavigne. None of the 35 current and former employees interviewed for the probe reported knowing of fraud, but the process did leave unanswered questions about image “anomalies” and brought an unrelated misconduct issue to public attention. In February, The Stanford Daily reported that an internal review “discovered falsification of data in the research” into the potential role of death receptor six (DR6) and amyloid precursor protein (APP) in Alzheimer’s disease, and claimed Tessier-Lavigne, Genentech’s former chief scientific officer, “kept the finding from becoming public.” The student-run newspaper ran a follow-up article last month after obtaining an email from a Stanford professor that said “there was discussion of fraud/fakery and MTL knew.” Genentech responded to the reports by conducting its own investigation. The findings (PDF) largely exonerate Tessier-Lavigne, now the president of Stanford, while still leaving loose ends that may simply reflect the challenges of investigating events that began around 15 years ago. Here’s the top-line positive finding for the accused: “None of the current or former employees who were interviewed reported observing or knowing of any fraud, fabrication, or other intentional wrongdoing in the research leading to and reported in the 2009 Nature paper.” Genentech was also unable to find any evidence that its Research Review Committee investigated fraud, fabrication or misconduct related to the work at the time, as was claimed in the original article. Other aspects of the review are less clear-cut. Genentech tasked “an independent, outside expert who specializes in detecting image manipulations in scientific publications” with looking at the paper. The expert found two sets of figures that include duplicate images and a Western blot panel that “appears to include a composite of two images.” “We have not determined how these anomalies occurred,” the report states. One challenge is that some of the original data and images are missing. Noting that the research took place nearly 15 years ago. Genentech said “some data and images were saved on electronic storage media that may no longer exist.” The report states “Genentech scientists and research associates had difficulty reproducing certain results reported in the 2009 Nature paper, in particular, the binding interaction between DR6 and N-APP.” Genentech researchers not involved in the 2009 paper achieved inconsistent results when they tried to replicate the study, an issue that some of them attributed to “the purity and quality of the reagents used.” The inconsistency was evident prior to publication and persisted across three years of research. “Senior leaders at Genentech including Dr. Tessier-Lavigne knew of the inconsistent binding results, and there was uncertainty and speculation within the Genentech Research organization about why the binding interaction between DR6 and N-APP could not be reliably reproduced or confirmed,” the report states. After Tessier-Lavigne left Genentech, a senior leader in gRED, the biotech’s research unit, urged that the paper should be retracted or corrected in light of the inconsistent binding results. Only Tessier-Lavigne or another co-author could take such an action. Genentech decided to perform other experiments to evaluate binding and determine whether DR6 was a viable Alzheimer’s target. Ultimately, genetic experiments in two mouse models killed off the program. The experiments found amyloid plaques and other features of Alzheimer’s weren’t dependent on DR6, leading Genentech to stop work on the target in 2012. “Many scientists who worked on the project were disheartened by having devoted substantial time and energy to a program whose underlying biology was ultimately proven wrong. That sentiment gave rise to rumors about why the DR6 program failed,” the report states. The review did uncover a complaint “alleging scientific misconduct by another postdoc working in Dr. Tessier-Lavigne’s laboratory.” The complaint was dealt with at the time, leading to the termination of the postdoc’s employment and withdrawal of a manuscript. The complaint was unrelated to DR6.