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• W4220792557 abstract "Disrupting the methylation of telomeric silencing 1-like (DOT1L)-mediated histone H3 lysine 79 has been implicated in MLL fusion-mediated leukemogenesis. Recently, DOT1L has become an attractive therapeutic target for MLL-rearranged leukemias. Rigorous studies have been performed, and much progress has been achieved. Moreover, one DOT1L inhibitor, EPZ-5676, has entered clinical trials, but its clinical activity is modest. Here, we review the recent advances and future trends of various therapeutic strategies against DOT1L for MLL-rearranged leukemias, including DOT1L enzymatic activity inhibitors, DOT1L degraders, protein-protein interaction (PPI) inhibitors, and combinatorial interventions. In addition, the limitations, challenges, and prospects of these therapeutic strategies are discussed. In summary, we present a general overview of DOT1L as a target in MLL-rearranged leukemias to provide valuable guidance for DOT1L-associated drug development in the future. Although a variety of DOT1L enzymatic inhibitors have been identified, most of them require further optimization. Recent advances in the development of small molecule degraders, including heterobifunctional degraders and molecular glues, provide valuable insights and references for DOT1L degraders. However, drug R&D strategies and platforms need to be developed and preclinical experiments need to be performed with the purpose of blocking DOT1L-associated PPIs. DOT1L epigenetic-based combination therapy is worth considering and exploring, but the therapy should be based on a thorough understanding of the regulatory mechanism of DOT1L epigenetic modifications." @default.
• W4220792557 created "2022-04-03" @default.
• W4220792557 creator A5031150824 @default.
• W4220792557 creator A5037259538 @default.
• W4220792557 date "2022-03-24" @default.
• W4220792557 modified "2023-10-16" @default.
• W4220792557 title "Targeting the histone H3 lysine 79 methyltransferase DOT1L in MLL-rearranged leukemias" @default.
• W4220792557 cites W1560166507 @default.
• W4220792557 cites W1565539350 @default.
• W4220792557 cites W1620051969 @default.
• W4220792557 cites W1969355036 @default.
• W4220792557 cites W1975258216 @default.
• W4220792557 cites W1976033223 @default.
• W4220792557 cites W1977729188 @default.
• W4220792557 cites W1982457292 @default.
• W4220792557 cites W1989558233 @default.
• W4220792557 cites W1993790725 @default.
• W4220792557 cites W2004761725 @default.
• W4220792557 cites W2012147370 @default.
• W4220792557 cites W2014880942 @default.
• W4220792557 cites W2015493376 @default.
• W4220792557 cites W2026576443 @default.
• W4220792557 cites W2032252581 @default.
• W4220792557 cites W2037856618 @default.
• W4220792557 cites W2044682579 @default.
• W4220792557 cites W2051888282 @default.
• W4220792557 cites W2056179278 @default.
• W4220792557 cites W2059171174 @default.
• W4220792557 cites W2059382988 @default.
• W4220792557 cites W2063738914 @default.
• W4220792557 cites W2073652391 @default.
• W4220792557 cites W2074347699 @default.
• W4220792557 cites W2075756021 @default.
• W4220792557 cites W2076856442 @default.
• W4220792557 cites W2087188627 @default.
• W4220792557 cites W2091208410 @default.
• W4220792557 cites W2099980194 @default.
• W4220792557 cites W2103233056 @default.
• W4220792557 cites W2104082208 @default.
• W4220792557 cites W2108498698 @default.
• W4220792557 cites W2112075818 @default.
• W4220792557 cites W2116860088 @default.
• W4220792557 cites W2129651142 @default.
• W4220792557 cites W2130020386 @default.
• W4220792557 cites W2144100406 @default.
• W4220792557 cites W2160363772 @default.
• W4220792557 cites W2162520885 @default.
• W4220792557 cites W2164959344 @default.
• W4220792557 cites W2192121806 @default.
• W4220792557 cites W2205700110 @default.
• W4220792557 cites W2238355570 @default.
• W4220792557 cites W2291775912 @default.
• W4220792557 cites W2292096944 @default.
• W4220792557 cites W2296658645 @default.
• W4220792557 cites W2414968032 @default.
• W4220792557 cites W2415007519 @default.
• W4220792557 cites W2437490503 @default.
• W4220792557 cites W2470096999 @default.
• W4220792557 cites W2554624179 @default.
• W4220792557 cites W2587615823 @default.
• W4220792557 cites W2588056590 @default.
• W4220792557 cites W2590885695 @default.
• W4220792557 cites W2591778276 @default.
• W4220792557 cites W2592787461 @default.
• W4220792557 cites W2604326584 @default.
• W4220792557 cites W2605404244 @default.
• W4220792557 cites W2762064638 @default.
• W4220792557 cites W2774533007 @default.
• W4220792557 cites W2784108533 @default.
• W4220792557 cites W2792453707 @default.
• W4220792557 cites W2793212766 @default.
• W4220792557 cites W2794180511 @default.
• W4220792557 cites W2802129476 @default.
• W4220792557 cites W2884450929 @default.
• W4220792557 cites W2887168173 @default.
• W4220792557 cites W2893619628 @default.
• W4220792557 cites W2898278445 @default.
• W4220792557 cites W2913118546 @default.
• W4220792557 cites W2913126315 @default.
• W4220792557 cites W2917149656 @default.
• W4220792557 cites W2931320842 @default.
• W4220792557 cites W2939146474 @default.
• W4220792557 cites W2948961954 @default.
• W4220792557 cites W2954020213 @default.
• W4220792557 cites W2969682556 @default.
• W4220792557 cites W2974637121 @default.
• W4220792557 cites W2993378407 @default.
• W4220792557 cites W2993435749 @default.
• W4220792557 cites W2993552587 @default.
• W4220792557 cites W2998180590 @default.
• W4220792557 cites W2998302660 @default.
• W4220792557 cites W3007043319 @default.
• W4220792557 cites W3027679488 @default.
• W4220792557 cites W3035937900 @default.
• W4220792557 cites W3085362629 @default.
• W4220792557 cites W3092891279 @default.
• W4220792557 cites W3093166440 @default.
• W4220792557 cites W3112514862 @default.
• W4220792557 cites W3123057917 @default.
• W4220792557 cites W3130648111 @default.

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