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Structural basis for transcription factor ZBTB7A recognition of DNA and effects of ZBTB7A somatic mutations that occur in human acute myeloid leukemia. | LitMetric

AI Article Synopsis

  • - ZBTB7A is one of three related transcription factors in humans (ZBTB7A, B, and C) that help control gene transcription involved in processes like blood cell formation, cancer development, and metabolism, particularly glycolysis.
  • - These transcription factors have distinct DNA-binding domains and form specific connections with DNA sequences, particularly binding to motifs like G(a/c)CCC, which are crucial for their function.
  • - In research focused on mutations in ZBTB7A linked to acute myeloid leukemia, it was found that most mutations hinder DNA binding, particularly those in the first two zinc-finger domains, which could also provide insights into the functions of ZBTB7B and ZBTB7C

Article Abstract

ZBTB7A belongs to a small family of transcription factors having three members in humans (7A, 7B, and 7C). They share a BTB/POZ protein interaction domain at the amino end and a zinc-finger DNA-binding domain at the carboxyl end. They control the transcription of a wide range of genes, having varied functions in hematopoiesis, oncogenesis, and metabolism (in particular glycolysis). ZBTB7A-binding profiles at gene promoters contain a consensus G(a/c)CCC motif, followed by a CCCC sequence in some instances. Structural and mutational investigations suggest that DNA-specific contacts with the four-finger tandem array of ZBTB7A are formed sequentially, initiated from ZF1-ZF2 binding to G(a/c)CCC before spreading to ZF3-ZF4, which bind the DNA backbone and the 3' CCCC sequence, respectively. Here, we studied some mutations found in t(8;21)-positive acute myeloid leukemia patients that occur within the ZBTB7A DNA-binding domain. We determined that these mutations generally impair ZBTB7A DNA binding, with the most severe disruptions resulting from mutations in ZF1 and ZF2, and the least from a frameshift mutation in ZF3 that results in partial mislocalization. Information provided here on ZBTB7A-DNA interactions is likely applicable to ZBTB7B/C, which have overlapping functions with ZBTB7A in controlling primary metabolism.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9932118PMC
http://dx.doi.org/10.1016/j.jbc.2023.102885DOI Listing

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