| Literature DB >> 31068932 |
Abstract
Stem Cell Antigen-1 (Sca-1/Ly6A) was the first identified member of the Lymphocyte antigen-6 (Ly6) gene family. Sca-1 serves as a marker of cancer stem cells and tissue resident stem cells in mice. The Sca-1 gene is located on mouse chromosome 15. While a direct homolog of Sca-1 in humans is missing, human chromosome 8-the syntenic region to mouse chromosome 15-harbors several genes containing the characteristic domain known as LU domain. The function of the LU domain in human LY6 gene family is not yet defined. The LY6 gene family proteins are present on human chromosome 6, 8, 11, and 19. The most interesting of these genes are located on chromosome 8q24.3, a frequently amplified locus in human cancer. Human LY6 genes represent novel biomarkers for poor cancer prognosis and are required for cancer progression in addition to playing an important role in immune escape. Although the mechanism associated with these phenotype is not yet clear, it is timely to review the current literature in order to address the critical need for future advancements in this field. This review will summarize recent findings which describe the role of human LY6 genes-LY6D, LY6E, LY6H, LY6K, PSCA, LYPD2, SLURP1, GML, GPIHBP1, and LYNX1; and their orthologs in mice at chromosome 15.Entities:
Keywords: Immune; LY6D; LY6E; LY6H; LY6K; Oncology; TGF-β
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Year: 2019 PMID: 31068932 PMCID: PMC6491625 DOI: 10.3389/fimmu.2019.00819
Source DB: PubMed Journal: Front Immunol ISSN: 1664-3224 Impact factor: 7.561
The phenotype of knockout mice model of Ly6 gene family members.
| Ly6E | Ly6E | Embryonic lethal due to placental defect | SynTA receptor pathway |
| Ly6K | Ly6K | Viable adult male (infertile) and female (fertile) | Unknown |
| Lynx1 | Lynx1 | Viable adult mice with no apparent phenotype | Not Applicable |
| Slurp1 | Slurp1 | Viable adult mice with palmoplantar keratoderma, metabolic and neuromuscular abnormal phenotype | Unknown |
| GPIHBP1 | GPIHBP1 | Viable adult mice with hypertriglyceridemia phenotype | Lipolysis pathway |
The mouse Ly6 genes namely Ly6E, Ly6K, Slurp1, Lynx1, and Gpihbp1 have mouse orthologs and they have knockout mice described. The mouse Ly6 genes namely Pcsa, Lypd2, Ly6D, Gml, and Ly6H have human orthologs but the knockout mice have not been described. The mouse Ly6 genes Sca1, Ly6I/M, Ly6C1, Ly6C2, Ly6B, Ly6G, BC025446, 9030619P08Rik don't have human orthologs. Among these genes only Sca1 has been described in a knockout mice model.
Correlation of high mRNA expression and patient survival outcome in multiple cancer types.
| Ovarian | LY6D | Up | Poor prognosis |
| LY6E | Up | Poor prognosis | |
| LY6H | Up | Poor prognosis | |
| LY6K | Up | Poor prognosis | |
| Colorectal | LY6D | Up | Poor prognosis |
| LY6E | Up | Poor prognosis | |
| LY6H | Up | Poor prognosis | |
| LY6K | Up | Poor prognosis | |
| Gastric | LY6D | Up | Poor prognosis |
| LY6E | Up | Poor prognosis | |
| LY6H | Up | Poor prognosis | |
| LY6K | Up | Poor prognosis | |
| Breast | LY6D | Up | Poor prognosis |
| LY6E | Up | Poor prognosis | |
| LY6H | Up | Poor prognosis | |
| LY6K | Up | Poor prognosis | |
| Lung | LY6D | Up | Poor prognosis |
| LY6E | Up | Poor prognosis | |
| LY6H | Up | OS (NS), Others (NA) | |
| LY6K | Up | Poor prognosis | |
| Bladder | LY6D | Up | OS (NS), Others (NA) |
| LY6E | Up | Poor prognosis | |
| LY6H | NS | OS (NS), Others (NA) | |
| LY6K | Up | Poor prognosis | |
| Brain and CNS | LY6D | Up | OS (NS), Others (NA) |
| LY6E | Up | Poor prognosis | |
| LY6H | Up | OS (NS), Others (NA) | |
| LY6K | Up | Poor prognosis | |
| Cervical | LY6D | Up | OS (NA), RFS (NS) |
| LY6E | Up | OS (NA), RFS (NS) | |
| LY6H | Up | OS (NA), RFS (NS) | |
| LY6K | Up | OS (NA), RFS (NS) | |
| Esophageal | LY6D | Up | OS (NS), Others (NA) |
| LY6E | Up | OS (NS), Others (NA) | |
| LY6H | Up | OS (NS), Others (NA) | |
| LY6K | Up | OS (NS), Others (NA) | |
| Head and neck | LY6D | Up | OS (NS), Others (NA) |
| LY6E | Up | OS (NS), Others (NA) | |
| LY6H | Up | OS (NS), Others (NA) | |
| LY6K | Up | OS (NS), Others (NA) | |
| Pancreatic | LY6D | Up | OS (NS), Others (NA) |
| LY6E | Up | OS (NS), Others (NA) | |
| LY6H | Up | OS (NS), Others (NA) | |
| LY6K | Up | OS (NS), Others (NA) |
Figure 1Increased LY6D mRNA expression in cancer and patient survival. High LY6D RNA expression leads to poor survival in (A) renal clear cell carcinoma, (B) pancreatic ductal adenocarcinoma. These data were recently added in Km plotter webtool from RNA seq pan cancer analysis (38).
Figure 2Increased LY6E mRNA expression in cancer and patient survival. High LY6E RNA expression leads to (A) poor survival in renal papillary cell carcinoma, (B) good prognosis for renal clear cell carcinoma, (C) poor survival in pancreatic ductal adenocarcinoma. These data were recently added in Km plotter webtool from RNA seq pan cancer analysis (38).
Figure 3Increased LY6H mRNA expression in cancer and patient survival. High LY6H RNA expression leads to poor survival in (A) renal clear cell carcinoma, (B) pancreatic ductal adenocarcinoma (38).
Figure 4Increased LY6K mRNA expression in cancer and patient survival. High Ly6K RNA expression leads to poor survival in (A) renal clear cell carcinoma, (B) renal papillary cell carcinoma and, (C) pancreatic ductal adenocarcinoma (38).
Figure 5Network analysis of Ly6D, Ly6E, Ly6K, and Ly6H genes. (A) Pathway studio network analysis showed that LY6 signaling is involved in broad range of molecules including growth factor, nuclear receptor, and micro RNAs. The upstream regulators are not highlighted, the downstream effectors are highlighted with blue, and the potential binding partners are highlighted with green. (B) Pathway studio network analysis showed that Ly6 gene family affect multitude of cellular fate and cell-cell interaction with microenvironment ranging from growth, apoptosis, autophagy, immune response (37).