SemOpenAlex |

SemOpenAlex

Matches in SemOpenAlex for { <https://semopenalex.org/work/W4386884773> ?p ?o ?g. }

Showing items 1 to 100 of ±211 with 100 items per page.

W4386884773 endingPage "4651" @default.
W4386884773 startingPage "4651" @default.
W4386884773 abstract "The IRS (insulin receptor substrate) family of scaffold proteins includes insulin receptor substrate-4 (IRS4), which is expressed only in a few cell lines, including human kidney, brain, liver, and thymus and some cell lines. Its N-terminus carries a phosphotyrosine-binding (PTB) domain and a pleckstrin homology domain (PH), which distinguishes it as a member of this family. In this paper, we collected data about the molecular mechanisms that explain the relevance of IRS4 in the development of cancer and identify IRS4 differences that distinguish it from IRS1 and IRS2. Search engines and different databases, such as PubMed, UniProt, ENSEMBL and SCANSITE 4.0, were used. We used the name of the protein that it encodes “(IRS-4 or IRS4)”, or the combination of these terms with the word “(cancer)” or “(human)”, for searches. Terms related to specific tumor pathologies (“breast”, “ovary”, “colon”, “lung”, “lymphoma”, etc.) were also used. Despite the lack of knowledge on IRS4, it has been reported that some cancers and benign tumors are characterized by high levels of IRS-4 expression. Specifically, the role of IRS-4 in different types of digestive tract neoplasms, gynecological tumors, lung cancers, melanomas, hematological tumors, and other less common types of cancers has been shown. IRS4 differs from IRS1 and IRS2 in that can activate several oncogenes that regulate the PI3K/Akt cascade, such as BRK and FER, which are characterized by tyrosine kinase-like activity without regulation via extracellular ligands. In addition, IRS4 can activate the CRKL oncogene, which is an adapter protein that regulates the MAP kinase cascade. Knowledge of the role played by IRS4 in cancers at the molecular level, specifically as a platform for oncogenes, may enable the identification and validation of new therapeutic targets." @default.
W4386884773 created "2023-09-21" @default.
W4386884773 creator A5020649839 @default.
W4386884773 creator A5023696165 @default.
W4386884773 creator A5028827338 @default.
W4386884773 creator A5034166202 @default.
W4386884773 creator A5037356434 @default.
W4386884773 creator A5055450973 @default.
W4386884773 creator A5060738504 @default.
W4386884773 creator A5067940071 @default.
W4386884773 creator A5081585010 @default.
W4386884773 creator A5091339799 @default.
W4386884773 date "2023-09-20" @default.
W4386884773 modified "2023-10-18" @default.
W4386884773 title "Is Insulin Receptor Substrate4 (IRS4) a Platform Involved in the Activation of Several Oncogenes?" @default.
W4386884773 cites W1697523131 @default.
W4386884773 cites W1966402141 @default.
W4386884773 cites W1967675708 @default.
W4386884773 cites W1968812902 @default.
W4386884773 cites W1973934934 @default.
W4386884773 cites W1974740641 @default.
W4386884773 cites W1981072221 @default.
W4386884773 cites W1982479748 @default.
W4386884773 cites W1982642169 @default.
W4386884773 cites W1982799272 @default.
W4386884773 cites W1983513002 @default.
W4386884773 cites W1988476050 @default.
W4386884773 cites W1989324173 @default.
W4386884773 cites W1991314258 @default.
W4386884773 cites W2000623239 @default.
W4386884773 cites W2001416110 @default.
W4386884773 cites W2004331701 @default.
W4386884773 cites W2004622459 @default.
W4386884773 cites W2011793316 @default.
W4386884773 cites W2012307370 @default.
W4386884773 cites W2013578942 @default.
W4386884773 cites W2016796510 @default.
W4386884773 cites W2017181626 @default.
W4386884773 cites W2020888229 @default.
W4386884773 cites W2025059796 @default.
W4386884773 cites W2030232704 @default.
W4386884773 cites W2031504013 @default.
W4386884773 cites W2033009146 @default.
W4386884773 cites W2033429522 @default.
W4386884773 cites W2037468699 @default.
W4386884773 cites W2040063654 @default.
W4386884773 cites W2042121553 @default.
W4386884773 cites W2048522531 @default.
W4386884773 cites W2052645554 @default.
W4386884773 cites W2058620622 @default.
W4386884773 cites W2062689336 @default.
W4386884773 cites W2064801081 @default.
W4386884773 cites W2073733047 @default.
W4386884773 cites W2075291089 @default.
W4386884773 cites W2075645766 @default.
W4386884773 cites W2080308138 @default.
W4386884773 cites W2092817365 @default.
W4386884773 cites W2095692554 @default.
W4386884773 cites W2096913544 @default.
W4386884773 cites W2097369775 @default.
W4386884773 cites W2106329420 @default.
W4386884773 cites W2107826612 @default.
W4386884773 cites W2113520782 @default.
W4386884773 cites W2114279126 @default.
W4386884773 cites W2115449075 @default.
W4386884773 cites W2117068783 @default.
W4386884773 cites W2121311150 @default.
W4386884773 cites W2121646990 @default.
W4386884773 cites W2122393978 @default.
W4386884773 cites W2136400536 @default.
W4386884773 cites W2137052325 @default.
W4386884773 cites W2139419157 @default.
W4386884773 cites W2143859801 @default.
W4386884773 cites W2153056550 @default.
W4386884773 cites W2153554962 @default.
W4386884773 cites W2155530767 @default.
W4386884773 cites W2157547728 @default.
W4386884773 cites W2192892788 @default.
W4386884773 cites W2262314662 @default.
W4386884773 cites W2381569410 @default.
W4386884773 cites W2404359304 @default.
W4386884773 cites W2517957586 @default.
W4386884773 cites W2518658791 @default.
W4386884773 cites W2529607059 @default.
W4386884773 cites W2554129223 @default.
W4386884773 cites W2555451680 @default.
W4386884773 cites W2572242198 @default.
W4386884773 cites W2589233140 @default.
W4386884773 cites W2606553662 @default.
W4386884773 cites W2609444947 @default.
W4386884773 cites W2611202697 @default.
W4386884773 cites W2732508265 @default.
W4386884773 cites W2745908238 @default.
W4386884773 cites W2766084386 @default.
W4386884773 cites W2769303155 @default.
W4386884773 cites W2781525129 @default.
W4386884773 cites W2788637261 @default.
W4386884773 cites W2790680781 @default.