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• W2026794512 abstract "Abstract Loss of RB1 gene is considered either a causal or an accelerating event in retinoblastoma. A variety of mechanisms inactivates RB1 gene, including intragenic mutations, loss of expression by methylation and chromosomal deletions, with effects which are species–and cell type‐specific. RB1 deletion can even lead to aneuploidy thus greatly increasing cancer risk. The RB1gene is part of a larger gene family that includes RBL1 and RBL2, each of the three encoding structurally related proteins indicated as pRb, p107, and p130, respectively. The great interest in these genes and proteins springs from their ability to slow down neoplastic growth. pRb can associate with various proteins by which it can regulate a great number of cellular activities. In particular, its association with the E2F transcription factor family allows the control of the main pRb functions, while the loss of these interactions greatly enhances cancer development. As RB1 gene, also pRb can be functionally inactivated through disparate mechanisms which are often tissue specific and dependent on the scenario of the involved tumor suppressors and oncogenes. The critical role of the context is complicated by the different functions played by the RB proteins and the E2F family members. In this review, we want to emphasize the importance of the mechanisms of RB1/pRb inactivation in inducing cancer cell development. The review is divided in three chapters describing in succession the mechanisms of RB1 inactivation in cancer cells, the alterations of pRb pathway in tumorigenesis and the RB protein and E2F family in cancer. J. Cell. Physiol. 228: 1676–1687, 2013. © 2013 Wiley Periodicals, Inc." @default.
• W2026794512 created "2016-06-24" @default.
• W2026794512 creator A5023176385 @default.
• W2026794512 creator A5072453901 @default.
• W2026794512 creator A5080064542 @default.
• W2026794512 creator A5091875238 @default.
• W2026794512 date "2013-04-18" @default.
• W2026794512 modified "2023-10-16" @default.
• W2026794512 title "RB1 in cancer: Different mechanisms of RB1 inactivation and alterations of pRb pathway in tumorigenesis" @default.
• W2026794512 cites W14762771 @default.
• W2026794512 cites W1531681328 @default.
• W2026794512 cites W1635667563 @default.
• W2026794512 cites W1709607181 @default.
• W2026794512 cites W1814300263 @default.
• W2026794512 cites W1827831640 @default.
• W2026794512 cites W1833347037 @default.
• W2026794512 cites W1911118961 @default.
• W2026794512 cites W1923050340 @default.
• W2026794512 cites W1938171108 @default.
• W2026794512 cites W1964635246 @default.
• W2026794512 cites W1968777135 @default.
• W2026794512 cites W1974199078 @default.
• W2026794512 cites W1974258814 @default.
• W2026794512 cites W1981283223 @default.
• W2026794512 cites W1983028272 @default.
• W2026794512 cites W1983287898 @default.
• W2026794512 cites W1984252723 @default.
• W2026794512 cites W1987699520 @default.
• W2026794512 cites W1991595805 @default.
• W2026794512 cites W1992125279 @default.
• W2026794512 cites W1992450235 @default.
• W2026794512 cites W1993323102 @default.
• W2026794512 cites W1995776632 @default.
• W2026794512 cites W1998174102 @default.
• W2026794512 cites W2000649021 @default.
• W2026794512 cites W2000965640 @default.
• W2026794512 cites W2013863113 @default.
• W2026794512 cites W2015003540 @default.
• W2026794512 cites W2018956184 @default.
• W2026794512 cites W2021522009 @default.
• W2026794512 cites W2024908788 @default.
• W2026794512 cites W2025461214 @default.
• W2026794512 cites W2026325417 @default.
• W2026794512 cites W2029487801 @default.
• W2026794512 cites W2031755356 @default.
• W2026794512 cites W2034277114 @default.
• W2026794512 cites W2034440981 @default.
• W2026794512 cites W2035546645 @default.
• W2026794512 cites W2036523261 @default.
• W2026794512 cites W2036642101 @default.
• W2026794512 cites W2036981111 @default.
• W2026794512 cites W2037296062 @default.
• W2026794512 cites W2037764323 @default.
• W2026794512 cites W2039272485 @default.
• W2026794512 cites W2040408498 @default.
• W2026794512 cites W2040611199 @default.
• W2026794512 cites W2041597883 @default.
• W2026794512 cites W2044242141 @default.
• W2026794512 cites W2044588337 @default.
• W2026794512 cites W2047506741 @default.
• W2026794512 cites W2052897800 @default.
• W2026794512 cites W2052912081 @default.
• W2026794512 cites W2057489420 @default.
• W2026794512 cites W2057720777 @default.
• W2026794512 cites W2060084956 @default.
• W2026794512 cites W2064241321 @default.
• W2026794512 cites W2065066575 @default.
• W2026794512 cites W2065906581 @default.
• W2026794512 cites W2068037892 @default.
• W2026794512 cites W2069678419 @default.
• W2026794512 cites W2071703458 @default.
• W2026794512 cites W2075279572 @default.
• W2026794512 cites W2075532269 @default.
• W2026794512 cites W2076273397 @default.
• W2026794512 cites W2077858999 @default.
• W2026794512 cites W2078047503 @default.
• W2026794512 cites W2078066154 @default.
• W2026794512 cites W2083187335 @default.
• W2026794512 cites W2084171824 @default.
• W2026794512 cites W2088085220 @default.
• W2026794512 cites W2088182309 @default.
• W2026794512 cites W2091066174 @default.
• W2026794512 cites W2094299510 @default.
• W2026794512 cites W2095689320 @default.
• W2026794512 cites W2096198457 @default.
• W2026794512 cites W2099282022 @default.
• W2026794512 cites W2099742439 @default.
• W2026794512 cites W2104660346 @default.
• W2026794512 cites W2104713031 @default.
• W2026794512 cites W2109651348 @default.
• W2026794512 cites W2113444840 @default.
• W2026794512 cites W2114388543 @default.
• W2026794512 cites W2115895726 @default.
• W2026794512 cites W2116738722 @default.
• W2026794512 cites W2118866877 @default.
• W2026794512 cites W2120491114 @default.
• W2026794512 cites W2122039072 @default.
• W2026794512 cites W2122129374 @default.

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