CD261 _ TRAIL_R1

Price:

185.71 €

Known as:: CD261 _ TRAIL_R1
Catalog number:: 10-403-C025
Product Quantity:: 0.025 mg
Category:: -
Supplier:: Exbio
Gene target:: CD261 _ TRAIL_R1

Related genes to: CD261 _ TRAIL_R1

Gene:: TNFRSF10A ^{NIH gene}
Name:: TNF receptor superfamily member 10a
Previous symbol:: -
Synonyms:: DR4, Apo2, TRAILR-1, CD261, TRAILR1
Chromosome:: 8p21.3
Locus Type:: gene with protein product
Date approved:: 1998-12-04
Date modifiied:: 2018-01-25

Related products to: CD261 _ TRAIL_R1

Antagonist decoy receptor for TRAIL_Apo-2L,DcR1,DCR1,Decoy receptor 1,Decoy TRAIL receptor without death domain,Homo sapiens,Human,LIT,Lymphocyte inhibitor of TRAIL,TNF-related apoptosis-inducing ligaAnti- Rabbit Anti-Human DR5 (TRAIL-R2) AntibodyAnti-CD253/TRAIL Antibody (CT) Polyclonal Antibody (OAAI00454)Anti-CD253/TRAIL Antibody (IN1) Polyclonal Antibody (OAAI00452)Anti-CD253/TRAIL Antibody (IN2) Polyclonal Antibody (OAAI00453)Anti-Human CD253 (TRAIL) Biotin 100 ugAnti-Human CD253 (TRAIL) Biotin 25 ugAnti-Human CD253 (TRAIL) Functional Grade Purified 100 ugAnti-Human CD253 (TRAIL) PE 100 testsAnti-Human CD253 (TRAIL) PE 25 testsAnti-Human CD253 (TRAIL) Purified 100 ugAnti-Human CD253 (TRAIL) Purified 25 ugAnti-Human CD261 (DR4) Biotin 100 ugAnti-Human CD261 (DR4) Biotin 25 ugAnti-Human CD261 (DR4) PE 100 tests

Related articles to: CD261 _ TRAIL_R1

Targeting RELA and STAT3 regulates TNFRSF10A-mediated apoptosis in a novel apoptosis-based prognostic model for clear cell renal cell carcinoma.
Clear cell renal cell carcinoma (ccRCC) is the most common subtype of renal malignancy and remains a major cause of cancer-related mortality worldwide. Although advances in surgery, targeted therapy, and immunotherapy have improved outcomes for patients, reliable biomarkers for predicting prognosis remain limited. Therefore, robust gene-based prognostic models are urgently needed to improve risk stratification and guide individualized treatment strategies. - Source: PubMed
Publication date: 2026/06/22
Deng YuyouHao ChangzhenYang XiaobingYu ChengfanXia MingWang Tian
Targeted plasma proteomics reveals a central role of upregulated TNFRSF proteins in HIV-associated stroke.
Chronic inflammation drives vascular aging and stroke risk, yet circulating proteins linking immune activation to cerebrovascular events remain elusive. People with HIV (PWH) face elevated stroke risk beyond traditional vascular risk factors, even under antiretroviral therapy. We aimed to identify circulating proteomic signatures of HIV-associated stroke, characterize underlying biological pathways, and assess their longitudinal stability. We conducted a nested case-control study of 135 PWH with stroke (HIV + /Stroke + , mean age 64.2 years, 85.9% ischemic) and two matched control groups (HIV + /Stroke- and HIV - /Stroke - , n = 135 each), with longitudinal validation in 37 PWH who subsequently developed stroke (78.4% ischemic). Among 184 plasma proteins measured using Olink Cardiovascular panels, 16 were associated with stroke in PWH, centrally involving the tumor necrosis factor receptor superfamily (TNFRSF). TNFRSF proteins (TNFRSF10A, TRAIL-R2, TNFRSF14, and TNF-R1) were strongly inter-correlated (ρ > 0.77), with their co-expression module associated with stroke (adjusted OR = 1.75, P = 0.018). TNFRSF expression increased monotonically across HIV - /Stroke - , HIV + /Stroke - , and HIV + /Stroke+ groups. Longitudinal analysis confirmed post-stroke upregulation of these TNFRSF members, alongside MMP12 and TFF3, particularly in ischemic subtypes. These findings suggest coordinated TNFRSF upregulation as a potential signature associated with both HIV-related inflammation and cerebrovascular events, providing candidate biomarkers for future investigation. - Source: PubMed
Publication date: 2026/06/09
Chen TailinLin HaijiangChen XiaoxiaoWang MiaochenZhang HaijunWang ShanlingWang LiangyouWang TingtingXie YaliWang YatingRen JiyuanZhang ZhiyiHe Na
GWAS Meta-analysis Identifies Novel Associated Loci and Points to Causal Tissues in Central Serous Chorioretinopathy.
To define CSC genetic architecture and identify implicated ocular tissues, cell types, genes, and circulating proteins. - Source: PubMed
Publication date: 2026/05/22
Chen LiyinKim Soo HyunTruong BuuRämö Joel TGorman Bryan Rvan Dijk Elon H CBrinks JoostNikopensius TiitChoi Seung HoanKajanne RistoMehtonen JuhaKaarniranta KaiSobrin LuciaKurki MitjaYzer Suzanne Wu Wen-ChihTurunen Joni ASegrè Ayellet JMercader Josep MariaHuerta AliciaDaly Mark JPalotie AarnoEllinor Patrick TBoon Camiel JfIyengar Sudha KPeachey Neal SNatarajan PradeepRossin Elizabeth J
Circulating biomarker profile and its diagnostic predictive utility in age-related macular degeneration.
We evaluated the serum expression profiles of proteins encoded by AMD-related genes in age-related macular degeneration patients and controls. - Source: PubMed
Publication date: 2026/06/03
Battu PriyaSharma SureshSingh RamandeepAnand Akshay
Genetic and epidemiological analyses of alcohol consumption patterns and age-related macular degeneration risk among current drinkers: a role for TNFRSF10A.
Alcohol intake, a major modifiable lifestyle factor, has been variably associated with age-related macular degeneration (AMD). We aim to investigate the association and potential causal relevance of alcohol consumption with AMD risk using complementary epidemiological and genetic approaches. - Source: PubMed
Publication date: 2026/05/22
Shen TingLi JingYang XiongyiXia JiaoZhou HanMa QianWang YulingWang JiajiaWang ZhenhuaLiu KunYan Biao

CD261 _ TRAIL_R1

Related genes to: CD261 _ TRAIL_R1

Related products to: CD261 _ TRAIL_R1

Related articles to: CD261 _ TRAIL_R1

Targeting RELA and STAT3 regulates TNFRSF10A-mediated apoptosis in a novel apoptosis-based prognostic model for clear cell renal cell carcinoma.

Targeted plasma proteomics reveals a central role of upregulated TNFRSF proteins in HIV-associated stroke.

GWAS Meta-analysis Identifies Novel Associated Loci and Points to Causal Tissues in Central Serous Chorioretinopathy.

Circulating biomarker profile and its diagnostic predictive utility in age-related macular degeneration.

Genetic and epidemiological analyses of alcohol consumption patterns and age-related macular degeneration risk among current drinkers: a role for TNFRSF10A.