Impaired cell fate through gain-of-function mutations in a chromatin reader

Wan, Liling; Chong, Shasha; Xuan, Fan; Liang, Angela; Cui, Xiaodong; Gates, Leah; Carroll, Thomas; Li, Yuanyuan; Feng, Lijuan; Chen, Guochao; Wang, Shu Ping; Ortiz, Michael V.; Daley, Sara K.; Wang, Xiaolu; Xuan, Hongwen; Kentsis, Alex; Muir, Tom W.; Roeder, Robert G.; Li, Haitao; Li, Wei; Tjian, Robert; Wen, Hong; Allis, C. David

doi:10.1038/s41586-019-1842-7

Cited by 118 publications

(149 citation statements)

References 20 publications

Supporting

Mentioning

139

Contrasting

Unclassified

Order By: Relevance

“…Importantly, targeting this H3K4me3-specific reader could also be beneficial for coinciding blocking of all three oncogenic proteins. Histone readers are increasingly considered to be druggable, and a number of potent inhibitors of acetyllysine recognizing bromodomain and YEATS domain have been developed in the past 10 years [24][25][26][27] . The pioneering studies 8,9,22 uncovering the pivotal role of the histone binding by the PHD finger of KDM5A, PHF23, and BPTF in NUP98 fusions in leukemic transformation and the feasibility of targeting these fusions by small molecules together with our mechanistic findings further suggest that impairing the PHD finger function and/or structure may provide an effective way to treat AMLs associated with these NUP98 fusions.…”

Section: Resultsmentioning

confidence: 99%

Mechanistic insights into chromatin targeting by leukemic NUP98-PHF23 fusion

et al. 2020

View full text Add to dashboard Cite

Chromosomal NUP98-PHF23 translocation is associated with an aggressive form of acute myeloid leukemia (AML) and poor survival rate. Here, we report the molecular mechanisms by which NUP98-PHF23 recognizes the histone mark H3K4me3 and is inhibited by small molecule compounds, including disulfiram that directly targets the PHD finger of PHF23 (PHF23PHD). Our data support a critical role for the PHD fingers of NUP98-PHF23, and related NUP98-KDM5A and NUP98-BPTF fusions in driving leukemogenesis, and demonstrate that blocking this interaction in NUP98-PHF23 expressing AML cells leads to cell death through necrotic and late apoptosis pathways. An overlap of NUP98-KDM5A oncoprotein binding sites and H3K4me3-positive loci at the Hoxa/b gene clusters and Meis1 in ChIP-seq, together with NMR analysis of the H3K4me3-binding sites of the PHD fingers from PHF23, KDM5A and BPTF, suggests a common PHD finger-dependent mechanism that promotes leukemogenesis by this type of NUP98 fusions. Our findings highlight the direct correlation between the abilities of NUP98-PHD finger fusion chimeras to associate with H3K4me3enriched chromatin and leukemic transformation.

show abstract

Section: Resultsmentioning

confidence: 99%

Mechanistic insights into chromatin targeting by leukemic NUP98-PHF23 fusion

et al. 2020

View full text Add to dashboard Cite

show abstract

“…6e ). A recent study reported that oncogenic mutations of ENL identified in Wilms tumor drove aberrant gene transcription by enhancing self-association ability of ENL, and the self-association ability of ENL mutants relied on the IDR region and the ET (also called AHD) domain of ENL 32 . Thus, it is a general feature for YET-family proteins to form the central hub to concentrate many complexes to a compartmentalized unit for efficient transcription, reinforcing the notion that YET-family proteins are master transcriptional regulators in cells 3 , 14 – 16 .…”

Section: Discussionmentioning

confidence: 99%

Taf14 recognizes a common motif in transcriptional machineries and facilitates their clustering by phase separation

Chen

Wang

et al. 2020

Nat Commun

Self Cite

View full text Add to dashboard Cite

Saccharomyces cerevisiae TBP associated factor 14 (Taf14) is a well-studied transcriptional regulator that controls diverse physiological processes and that physically interacts with at least seven nuclear complexes in yeast. Despite multiple previous Taf14 structural studies, the nature of its disparate transcriptional regulatory functions remains opaque. Here, we demonstrate that the extra-terminal (ET) domain of Taf14 (Taf14 ET ) recognizes a common motif in multiple transcriptional coactivator proteins from several nuclear complexes, including RSC, SWI/SNF, INO80, NuA3, TFIID, and TFIIF. Moreover, we show that such partner binding promotes liquid-liquid phase separation (LLPS) of Taf14 ET , in a mechanism common to YEATS-associated ET domains (e.g., AF9 ET ) but not Bromo-associated ET domains from BET-family proteins. Thus, beyond identifying the molecular mechanism by which Taf14 ET associates with many transcriptional regulators, our study suggests that Taf14 may function as a versatile nuclear hub that orchestrates transcriptional machineries to spatiotemporally regulate diverse cellular pathways.

show abstract

“…Recurrent hot spot mutations have been found in ENL YEATS domain in WTs [ 208 ]. ENL protein is a reader of histone acetylation through its YEATS domain.…”

Section: Wilms Nephroblastomamentioning

confidence: 99%

“…ENL protein is a reader of histone acetylation through its YEATS domain. Using human and mouse cellular models, evidence was provided that ENL mutants induce gene expression changes that promote a premalignant condition and in nephrogenesis models induce the formation of undifferentiated cellular structures resembling those observed in WTs [ 208 ]. At mechanistic level, these ENL mutations exhibit a function similar to their normal counterpart, occupying similar target genomic loci, but with a clearly increased occupancy, leading to a pronounced increase in the recruitment and activity of transcription elongation machinery, thus enforcing the rate and the level of gene transcription of these target genes [ 208 ].…”

Section: Wilms Nephroblastomamentioning

confidence: 99%

Genetic Alterations in Renal Cancers: Identification of The Mechanisms Underlying Cancer Initiation and Progression and of Therapeutic Targets

Testa

Castelli

2020

Medicines

View full text Add to dashboard Cite

Renal cell cancer (RCC) involves three most recurrent sporadic types: clear-cell RCC (70–75%, CCRCC), papillary RCCC (10–15%, PRCC), and chromophobe RCC (5%, CHRCC). Hereditary cases account for about 5% of all cases of RCC and are caused by germline pathogenic variants. Herein, we review how a better understanding of the molecular biology of RCCs has driven the inception of new diagnostic and therapeutic approaches. Genomic research has identified relevant genetic alterations associated with each RCC subtype. Molecular studies have clearly shown that CCRCC is universally initiated by Von Hippel Lindau (VHL) gene dysregulation, followed by different types of additional genetic events involving epigenetic regulatory genes, dictating disease progression, aggressiveness, and differential response to treatments. The understanding of the molecular mechanisms that underlie the development and progression of RCC has considerably expanded treatment options; genomic data might guide treatment options by enabling patients to be matched with therapeutics that specifically target the genetic alterations present in their tumors. These new targeted treatments have led to a moderate improvement of the survival of metastatic RCC patients. Ongoing studies based on the combination of immunotherapeutic agents (immune check inhibitors) with VEGF inhibitors are expected to further improve the survival of these patients.

show abstract

Impaired cell fate through gain-of-function mutations in a chromatin reader

Cited by 118 publications

References 20 publications

Mechanistic insights into chromatin targeting by leukemic NUP98-PHF23 fusion

Mechanistic insights into chromatin targeting by leukemic NUP98-PHF23 fusion

Taf14 recognizes a common motif in transcriptional machineries and facilitates their clustering by phase separation

Genetic Alterations in Renal Cancers: Identification of The Mechanisms Underlying Cancer Initiation and Progression and of Therapeutic Targets

Contact Info

Product

Resources

About