SemOpenAlex |

SemOpenAlex

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2034244318> ?p ?o ?g. }

Showing items 1 to 100 of ±241 with 100 items per page.

W2034244318 endingPage "1406" @default.
W2034244318 startingPage "1396" @default.
W2034244318 abstract "Hematopoiesis is a tightly regulated process involving the control of gene expression that directs the transition from hematopoietic stem and progenitor cells to terminally differentiated blood cells. In leukemia, the processes directing self-renewal, differentiation and progenitor cell expansion are disrupted, leading to the accumulation of immature, non-functioning malignant cells. Insights into these processes have come in stages, based on technological advances in genetic analyses, bioinformatics and biological sciences. The first cytogenetic studies of leukemic cells identified chromosomal translocations that generate oncogenic fusion proteins and most commonly affect regulators of transcription. This was followed by the discovery of recurrent somatic mutations in genes encoding regulators of the signal transduction pathways that control cell proliferation and survival. Recently, studies of global changes in methylation and gene expression have led to the understanding that the output of transcriptional regulators and the proliferative signaling pathways are ultimately influenced by chromatin structure. Candidate gene, whole-genome and whole-exome sequencing studies have identified recurrent somatic mutations in genes encoding epigenetic modifiers in both acute myeloid leukemia (AML) and acute lymphoid leukemia (ALL). In contrast to the two-hit model of leukemogenesis, emerging evidence suggests that these epigenetic modifiers represent a class of mutations that are critical to the development of leukemia and affect the regulation of various other oncogenic pathways. In this review, we discuss the range of recurrent, somatic mutations in epigenetic modifiers found in leukemia and how these modifiers relate to the classical leukemogenic pathways that lead to impaired cell differentiation and aberrant self-renewal and proliferation." @default.
W2034244318 created "2016-06-24" @default.
W2034244318 creator A5020996374 @default.
W2034244318 creator A5089486443 @default.
W2034244318 date "2014-03-10" @default.
W2034244318 modified "2023-10-15" @default.
W2034244318 title "Chromatin modifiers and the promise of epigenetic therapy in acute leukemia" @default.
W2034244318 cites W1255676896 @default.
W2034244318 cites W1492609361 @default.
W2034244318 cites W174577041 @default.
W2034244318 cites W1963736125 @default.
W2034244318 cites W1964700896 @default.
W2034244318 cites W1966010937 @default.
W2034244318 cites W1968025025 @default.
W2034244318 cites W1968677867 @default.
W2034244318 cites W1968761707 @default.
W2034244318 cites W1969945914 @default.
W2034244318 cites W1971659434 @default.
W2034244318 cites W1972016428 @default.
W2034244318 cites W1974079495 @default.
W2034244318 cites W1974119365 @default.
W2034244318 cites W1974798829 @default.
W2034244318 cites W1975260788 @default.
W2034244318 cites W1975267683 @default.
W2034244318 cites W1975511102 @default.
W2034244318 cites W1976021347 @default.
W2034244318 cites W1976033223 @default.
W2034244318 cites W1976573435 @default.
W2034244318 cites W1977836335 @default.
W2034244318 cites W1978286333 @default.
W2034244318 cites W1978660434 @default.
W2034244318 cites W1978972655 @default.
W2034244318 cites W1979699800 @default.
W2034244318 cites W1981463058 @default.
W2034244318 cites W1981543052 @default.
W2034244318 cites W1982315838 @default.
W2034244318 cites W1984879354 @default.
W2034244318 cites W1988819329 @default.
W2034244318 cites W1990274230 @default.
W2034244318 cites W1990382868 @default.
W2034244318 cites W1990739246 @default.
W2034244318 cites W1991903960 @default.
W2034244318 cites W1992320498 @default.
W2034244318 cites W1993362540 @default.
W2034244318 cites W1994648009 @default.
W2034244318 cites W1998367819 @default.
W2034244318 cites W1999813105 @default.
W2034244318 cites W2000533693 @default.
W2034244318 cites W2002625908 @default.
W2034244318 cites W2004380688 @default.
W2034244318 cites W2004842295 @default.
W2034244318 cites W2005829971 @default.
W2034244318 cites W2008735740 @default.
W2034244318 cites W2008876829 @default.
W2034244318 cites W2012753533 @default.
W2034244318 cites W2015132841 @default.
W2034244318 cites W2015158272 @default.
W2034244318 cites W2017337160 @default.
W2034244318 cites W2017492512 @default.
W2034244318 cites W2021785548 @default.
W2034244318 cites W2023149772 @default.
W2034244318 cites W2024373518 @default.
W2034244318 cites W2024985626 @default.
W2034244318 cites W2025921758 @default.
W2034244318 cites W2026034797 @default.
W2034244318 cites W2028078153 @default.
W2034244318 cites W2028243804 @default.
W2034244318 cites W2031121711 @default.
W2034244318 cites W2033078160 @default.
W2034244318 cites W2034748898 @default.
W2034244318 cites W2035409103 @default.
W2034244318 cites W2037856618 @default.
W2034244318 cites W2038676786 @default.
W2034244318 cites W2039278049 @default.
W2034244318 cites W2040092511 @default.
W2034244318 cites W2041191257 @default.
W2034244318 cites W2041535798 @default.
W2034244318 cites W2046838777 @default.
W2034244318 cites W2047867594 @default.
W2034244318 cites W2048613921 @default.
W2034244318 cites W2048920286 @default.
W2034244318 cites W2051293191 @default.
W2034244318 cites W2051743028 @default.
W2034244318 cites W2053421436 @default.
W2034244318 cites W2053856108 @default.
W2034244318 cites W2054301876 @default.
W2034244318 cites W2059130068 @default.
W2034244318 cites W2059171174 @default.
W2034244318 cites W2059526410 @default.
W2034244318 cites W2060605982 @default.
W2034244318 cites W2060712252 @default.
W2034244318 cites W2062640733 @default.
W2034244318 cites W2062767772 @default.
W2034244318 cites W2062927905 @default.
W2034244318 cites W2063296278 @default.
W2034244318 cites W2065858628 @default.
W2034244318 cites W2066236650 @default.
W2034244318 cites W2069591815 @default.