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W4327654310 endingPage "55" @default.
W4327654310 startingPage "21" @default.
W4327654310 abstract "Regulated cell division is one of the fundamental phenomena which is the basis of all life on earth. Even a single base pair mutation in DNA leads to the production of the dysregulated protein that can have catastrophic consequences. Cell division is tightly controlled and orchestrated by proteins called cyclins and cyclin-dependent kinase (CDKs), which serve as licensing factors during different phases of cell division. Dysregulated cell division is one of the most important hallmarks of cancer and is commonly associated with a mutation in cyclins and CDKs along with tumor suppressor proteins. Therefore, targeting the component of the cell cycle which leads to these characteristics would be an effective strategy for treating cancers. Specifically, Cyclin-dependent kinases (CDKs) involved in cell cycle regulation have been identified to be overexpressed in many cancers. Many studies indicate that oncogenesis occurs in cancerous cells by the overactivity of different CDKs, which impact cell cycle progression and checkpoint dysregulation which is responsible for development of tumor. The development of CDK inhibitors has emerged as a promising and novel approach for cancer treatment in both solid and hematological malignancies. Some of the novel CDK inhibitors have shown remarkable results in clinical trials, such as-Ribociclib®, Palbociclib® and Abemaciclib®, which are CDK4/6 inhibitors and have received FDA approval for the treatment of breast cancer. In this chapter, we discuss the molecular mechanism through which cyclins and CDKs regulate cell cycle progression and the emergence of cyclins and CDKs as rational targets in cancer. We also discuss recent advances in developing CDK inhibitors, which have emerged as a novel class of inhibitors, and their associated toxicities in recent years." @default.
W4327654310 created "2023-03-18" @default.
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W4327654310 date "2023-01-01" @default.
W4327654310 modified "2023-10-18" @default.
W4327654310 title "Cyclin-dependent kinases in cancer: Role, regulation, and therapeutic targeting" @default.
W4327654310 cites W1483655365 @default.
W4327654310 cites W1527674890 @default.
W4327654310 cites W1544564404 @default.
W4327654310 cites W1549691519 @default.
W4327654310 cites W1638194466 @default.
W4327654310 cites W1656358829 @default.
W4327654310 cites W1903523058 @default.
W4327654310 cites W1928704095 @default.
W4327654310 cites W1966432984 @default.
W4327654310 cites W1970108163 @default.
W4327654310 cites W1971623971 @default.
W4327654310 cites W1974559056 @default.
W4327654310 cites W1975165604 @default.
W4327654310 cites W1975186639 @default.
W4327654310 cites W1982166284 @default.
W4327654310 cites W1985039245 @default.
W4327654310 cites W1990624451 @default.
W4327654310 cites W1991054314 @default.
W4327654310 cites W1994992878 @default.
W4327654310 cites W1996799079 @default.
W4327654310 cites W1996931025 @default.
W4327654310 cites W2000177056 @default.
W4327654310 cites W2001570690 @default.
W4327654310 cites W2003929899 @default.
W4327654310 cites W2006401070 @default.
W4327654310 cites W2015066175 @default.
W4327654310 cites W2015807143 @default.
W4327654310 cites W2016766601 @default.
W4327654310 cites W2017898416 @default.
W4327654310 cites W2024466111 @default.
W4327654310 cites W2029620430 @default.
W4327654310 cites W2029875848 @default.
W4327654310 cites W2031487445 @default.
W4327654310 cites W2033208702 @default.
W4327654310 cites W2037257739 @default.
W4327654310 cites W2037992356 @default.
W4327654310 cites W2038143768 @default.
W4327654310 cites W2041254889 @default.
W4327654310 cites W2042772659 @default.
W4327654310 cites W2044145281 @default.
W4327654310 cites W2044312503 @default.
W4327654310 cites W2045451529 @default.
W4327654310 cites W2046847991 @default.
W4327654310 cites W2048875557 @default.
W4327654310 cites W2048938594 @default.
W4327654310 cites W2055546731 @default.
W4327654310 cites W2055576683 @default.
W4327654310 cites W2058891255 @default.
W4327654310 cites W2060508679 @default.
W4327654310 cites W2063941959 @default.
W4327654310 cites W2066324910 @default.
W4327654310 cites W2070278756 @default.
W4327654310 cites W2073068681 @default.
W4327654310 cites W2074913300 @default.
W4327654310 cites W2075731214 @default.
W4327654310 cites W2075776549 @default.
W4327654310 cites W2077037832 @default.
W4327654310 cites W2084607632 @default.
W4327654310 cites W2085593164 @default.
W4327654310 cites W2087450388 @default.
W4327654310 cites W2088118120 @default.
W4327654310 cites W2089648262 @default.
W4327654310 cites W2100287099 @default.
W4327654310 cites W2101606325 @default.
W4327654310 cites W2104458086 @default.
W4327654310 cites W2109323481 @default.
W4327654310 cites W2110541112 @default.
W4327654310 cites W2114460232 @default.
W4327654310 cites W2119827462 @default.
W4327654310 cites W2121619780 @default.
W4327654310 cites W2125211913 @default.
W4327654310 cites W2126821691 @default.
W4327654310 cites W2128411785 @default.
W4327654310 cites W2129381867 @default.
W4327654310 cites W2130258750 @default.
W4327654310 cites W2130802358 @default.
W4327654310 cites W2131017274 @default.
W4327654310 cites W2131717330 @default.
W4327654310 cites W2133382697 @default.
W4327654310 cites W2137620209 @default.
W4327654310 cites W2139726922 @default.