Browse ESAM

Summary
SymbolESAM
Nameendothelial cell adhesion molecule
Aliases W117m; 2310008D05Rik; HUEL (C4orf1)-interacting protein; LP4791 protein; Endothelial cell-selective adhesion ......
Chromosomal Location11q24.2
External Links HGNC, NCBI, Ensembl, Uniprot, GeneCards
Content Basic function annotation.
> Subcellular Location, Domain and Function
> Gene Ontology
> KEGG and Reactome Pathway
> Subcellular Location, Domain and Function
 
Subcellular Location Cell junction, adherens junction Cell junction, tight junction Cell membrane Single-pass type I membrane protein
Domain PF07686 Immunoglobulin V-set domain
Function

Can mediate aggregation most likely through a homophilic molecular interaction.

> Gene Ontology
 
Biological Process GO:0007156 homophilic cell adhesion via plasma membrane adhesion molecules
GO:0050900 leukocyte migration
GO:0098742 cell-cell adhesion via plasma-membrane adhesion molecules
Molecular Function -
Cellular Component GO:0005923 bicellular tight junction
GO:0043296 apical junction complex
GO:0070160 occluding junction
> KEGG and Reactome Pathway
 
KEGG hsa04514 Cell adhesion molecules (CAMs)
hsa04670 Leukocyte transendothelial migration
Reactome R-HSA-202733: Cell surface interactions at the vascular wall
R-HSA-109582: Hemostasis
Summary
SymbolESAM
Nameendothelial cell adhesion molecule
Aliases W117m; 2310008D05Rik; HUEL (C4orf1)-interacting protein; LP4791 protein; Endothelial cell-selective adhesion ......
Chromosomal Location11q24.2
External Links HGNC, NCBI, Ensembl, Uniprot, GeneCards
Content Literatures that report relations between ESAM and anti-tumor immunity. The specific mechanism were also collected if the literature reports that a gene specifically promotes or inhibits the infiltration or function of T/NK cells.
> Text Mining
 

There is no record.

Summary
SymbolESAM
Nameendothelial cell adhesion molecule
Aliases W117m; 2310008D05Rik; HUEL (C4orf1)-interacting protein; LP4791 protein; Endothelial cell-selective adhesion ......
Chromosomal Location11q24.2
External Links HGNC, NCBI, Ensembl, Uniprot, GeneCards
Content High-throughput screening data (e.g. CRISPR-Cas9, shRNA and RNAi) for T cell-mediated killing. Genetic screen techniques can identify mechanisms of tumor cell resistance (e.g., PTPN2) and sensitivity (e.g., APLNR) to killing by cytotoxic T cells, the central effectors of anti-tumor immunity. After comprehensively searching, eight groups of screening data sets were collected in the current database. In this tab, users can check whether their selected genes cause resistance or increase sensitivity to T cell-mediated killing in various data sets.
> High-throughput Screening
  Statistical results of ESAM in screening data sets for detecting immune reponses.
PMID Screening System Cancer Type Cell Line Data Set Statistical Results Relation to immunity
29301958CRISPR-Cas9 melanomaB16F10Pmel-1 T cell NA/NSNA/NS
29301958CRISPR-Cas9 melanomaB16F10OT-1 T cell NA/NSNA/NS
28783722CRISPR-Cas9 melanomaMel6242CT-CRISPR NA/NSNA/NS
28723893CRISPR-Cas9 melanomaB16GVAX+Anti-PD1 NA/NSNA/NS
28723893CRISPR-Cas9 melanomaB16GVAX NA/NSNA/NS
25691366RNAiBreast cancerMCF7Luc-CTL assay NA/NSNA/NS
24476824shRNAmelanomaB16Primary screen NA/NSNA/NS
24476824shRNAmelanomaB16Secondary screen NA/NSNA/NS
Summary
SymbolESAM
Nameendothelial cell adhesion molecule
Aliases W117m; 2310008D05Rik; HUEL (C4orf1)-interacting protein; LP4791 protein; Endothelial cell-selective adhesion ......
Chromosomal Location11q24.2
External Links HGNC, NCBI, Ensembl, Uniprot, GeneCards
Content Transcriptomic and genomic profiling of pre-treated tumor biopsies from responders and non-responders to immunotherapy. These data were used to identify signatures and mechanisms of response to checkpoint blockade (e.g., anti-PDL1 and anti-PD1). One example is that mutations in the gene PBRM1 benefit clinical survival of patients with clear cell renal cell carcinoma. After comprehensively searching, we collected 5 and 6 of transcriptomic and genomic data sets, respectively. In this tab, users can check whether their selected genes have significant difference of expression or mutation between responders and non-responders in various data sets.
> Expression difference between responders and non-responders
> Mutation difference between responders and non-responders
> Expression difference between responders and non-responders
 
Points in the above scatter plot represent the expression difference of ESAM in various data sets.
No PMID Cancer type Group Drug # Res # NRes Log2 (Fold Change) P value Anno
126997480MelanomaallAnti-PD-1 (pembrolizumab and nivolumab)1412-0.7860.0226
226997480MelanomaMAPKiAnti-PD-1 (pembrolizumab and nivolumab)65-0.7380.67
326997480Melanomanon-MAPKiAnti-PD-1 (pembrolizumab and nivolumab)87-0.8160.498
428552987Urothelial cancerallAnti-PD-L1 (atezolizumab) 9160.3430.341
528552987Urothelial cancersmokingAnti-PD-L1 (atezolizumab) 59-0.0710.97
628552987Urothelial cancernon-smokingAnti-PD-L1 (atezolizumab) 470.8610.704
729033130MelanomaallAnti-PD-1 (nivolumab) 26230.2670.485
829033130MelanomaNIV3-PROGAnti-PD-1 (nivolumab) 15110.3650.743
929033130MelanomaNIV3-NAIVEAnti-PD-1 (nivolumab) 11120.1320.917
1029301960Clear cell renal cell carcinoma (ccRCC)allAnti-PD-1 (nivolumab) 481.2590.543
1129301960Clear cell renal cell carcinoma (ccRCC)VEGFRiAnti-PD-1 (nivolumab) 2001
1229301960Clear cell renal cell carcinoma (ccRCC)non-VEGFRiAnti-PD-1 (nivolumab) 282.3640.415
1329443960Urothelial cancerallAnti-PD-L1 (atezolizumab) 68230-0.1360.203
> Mutation difference between responders and non-responders
 
Points in the above scatter plot represent the mutation difference of ESAM in various data sets.
No PMID Cancer type Group Drug # Res # NRes % Mut/Res % Mut/NRes % Diff (R vs NR) Pval Anno
125765070Non-small cell lung cancer (NSCLC)allAnti-PD-1 (pembrolizumab) 14177.107.10.452
225765070Non-small cell lung cancer (NSCLC)smokingAnti-PD-1 (pembrolizumab) 103100101
325765070Non-small cell lung cancer (NSCLC)non-smokingAnti-PD-1 (pembrolizumab) 4140001
426359337MelanomaallAnti-CTLA-4 (ipilimumab) 27733.72.711
526359337MelanomaBRAFiAnti-CTLA-4 (ipilimumab) 0140001
626359337Melanomanon-BRAFiAnti-CTLA-4 (ipilimumab) 27593.73.40.31
726997480MelanomaallAnti-PD-1 (pembrolizumab and nivolumab)21174.804.81
826997480MelanomaMAPKiAnti-PD-1 (pembrolizumab and nivolumab)860001
926997480Melanomanon-MAPKiAnti-PD-1 (pembrolizumab and nivolumab)13117.707.71
1028552987Urothelial cancerallAnti-PD-L1 (atezolizumab) 91606.2-6.21
1128552987Urothelial cancersmokingAnti-PD-L1 (atezolizumab) 59011.1-11.11
1228552987Urothelial cancernon-smokingAnti-PD-L1 (atezolizumab) 470001
1329033130MelanomaallAnti-PD-1 (nivolumab) 38270001
1429033130MelanomaNIV3-PROGAnti-PD-1 (nivolumab) 22130001
1529033130MelanomaNIV3-NAIVEAnti-PD-1 (nivolumab) 16140001
1629301960Clear cell renal cell carcinoma (ccRCC)allAnti-PD-1 (nivolumab) 11130001
1729301960Clear cell renal cell carcinoma (ccRCC)VEGFRiAnti-PD-1 (nivolumab) 610001
1829301960Clear cell renal cell carcinoma (ccRCC)non-VEGFRiAnti-PD-1 (nivolumab) 5120001
Summary
SymbolESAM
Nameendothelial cell adhesion molecule
Aliases W117m; 2310008D05Rik; HUEL (C4orf1)-interacting protein; LP4791 protein; Endothelial cell-selective adhesion ......
Chromosomal Location11q24.2
External Links HGNC, NCBI, Ensembl, Uniprot, GeneCards
Content Relations between abundance of tumor-infiltrating lymphocytes (TILs) and expression, copy number, methylation, or mutation of ESAM. The immune-related signatures of 28 TIL types from Charoentong's study, which can be viewed in the download page. For each cancer type, the relative abundance of TILs were inferred by using gene set variation analysis (GSVA) based on gene expression profile. In this tab, users can examine which kinds of TILs might be regulated by the current gene.
> Lymphocyte
 
Summary
SymbolESAM
Nameendothelial cell adhesion molecule
Aliases W117m; 2310008D05Rik; HUEL (C4orf1)-interacting protein; LP4791 protein; Endothelial cell-selective adhesion ......
Chromosomal Location11q24.2
External Links HGNC, NCBI, Ensembl, Uniprot, GeneCards
Content Relations between three kinds of immunomodulators and expression, copy number, methylation, or mutation of ESAM. These immunomo-dulators were collected from Charoentong's study. In this tab, users can examine which immunomodulators might be regulated by ESAM.
> Immunoinhibitor
> Immunostimulator
> MHC molecule
> Immunoinhibitor
 
> Immunostimulator
 
> MHC molecule
 
Summary
SymbolESAM
Nameendothelial cell adhesion molecule
Aliases W117m; 2310008D05Rik; HUEL (C4orf1)-interacting protein; LP4791 protein; Endothelial cell-selective adhesion ......
Chromosomal Location11q24.2
External Links HGNC, NCBI, Ensembl, Uniprot, GeneCards
Content Relations between chemokines (or receptors) and expression, copy number, methylation, or mutation of ESAM. In this tab, users can examine which chemokines (or receptors) might be regulated by the current gene.
> Chemokine
> Receptor
> Chemokine
 
> Receptor
 
Summary
SymbolESAM
Nameendothelial cell adhesion molecule
Aliases W117m; 2310008D05Rik; HUEL (C4orf1)-interacting protein; LP4791 protein; Endothelial cell-selective adhesion ......
Chromosomal Location11q24.2
External Links HGNC, NCBI, Ensembl, Uniprot, GeneCards
Content Distribution of ESAM expression across immune and molecular subtypes.
> Immune subtype
> Molecular subtype
> Immune subtype
 
> Molecular subtype
 
Summary
SymbolESAM
Nameendothelial cell adhesion molecule
Aliases W117m; 2310008D05Rik; HUEL (C4orf1)-interacting protein; LP4791 protein; Endothelial cell-selective adhesion ......
Chromosomal Location11q24.2
External Links HGNC, NCBI, Ensembl, Uniprot, GeneCards
Content Associations between ESAM and clinical features.
> Overall survival analysis
> Cancer stage
> Tumor grade
> Overall survival
 
> Stage
 
> Grade
 
Summary
SymbolESAM
Nameendothelial cell adhesion molecule
Aliases W117m; 2310008D05Rik; HUEL (C4orf1)-interacting protein; LP4791 protein; Endothelial cell-selective adhesion ......
Chromosomal Location11q24.2
External Links HGNC, NCBI, Ensembl, Uniprot, GeneCards
Content Drugs targeting ESAM collected from DrugBank database.
> Drugs from DrugBank database
 

There is no record.