Generation of Mice Deficient in both KLF3/BKLF and KLF8 Reveals a Genetic Interaction and a Role for These Factors in Embryonic Globin Gene Silencing

Funnell, Alister P. W.; Mak, Ka Sin; Twine, Natalie A.; Pelka, Gregory J.; Norton, Laura J.; Radziewic, Tania; Power, Melinda; Wilkins, Marc R.; Bell-Anderson, Kim; Fraser, Stuart T.; Perkins, Andrew C.; Tam, Patrick; Pearson, Richard; Crossley, Merlin

doi:10.1128/mcb.00074-13

Cited by 41 publications

(32 citation statements)

References 107 publications

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“…However, it has recently been shown that 2 members of the KLF family (KLF3 and KLF8) may be involved in regulating embryonic globin expression, and a knockout of these 2 transcription factors in erythroid cells de-represses embryonic globin synthesis. 41 Because expression of these 2 factors is driven by KLF1, it is possible that mutations in this protein might reduce KLF3 and KLF8, leading to derepression of embryonic globins. Further analysis of this pathway is warranted because preliminary studies in mice suggest that persistence of embryonic globin expression could ameliorate severe hemoglobinothathies.…”

Section: Discussionmentioning

confidence: 99%

Mutations in Krüppel-like factor 1 cause transfusion-dependent hemolytic anemia and persistence of embryonic globin gene expression

Viprakasit¹,

Ekwattanakit

Riolueang

et al. 2014

Blood

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Section: Discussionmentioning

confidence: 99%

Mutations in Krüppel-like factor 1 cause transfusion-dependent hemolytic anemia and persistence of embryonic globin gene expression

Viprakasit¹,

Ekwattanakit

Riolueang

et al. 2014

Blood

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“…CtBP2 interacts with the N-terminus of KLF3 and related KLFs to provide a repressor function. 71 Mice lacking both Klf3 and Klf8 fail to repress embryonic globin gene expression in vivo, 72 so regulation of CtBP2 could be an alternative mechanism by which KLF1 indirectly regulates embryonic and fetal globin gene silencing (ie, via "enabling" the repression functions of KLF3 and KLF8). We also found that KLF1 regulates SOX6, which plays a key role in definitive erythropoiesis and embryonic globin gene silencing.…”

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confidence: 99%

KLF1-null neonates display hydrops fetalis and a deranged erythroid transcriptome

Magor

Tallack

Gillinder

et al. 2015

Blood

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Key Points• Complete loss of KLF1 function is compatible with life but results in severe nonspherocytic hemolytic anemia and kernicterus.• Human KLF1 regulates most aspects of red cell biology.We describe a case of severe neonatal anemia with kernicterus caused by compound heterozygosity for null mutations in KLF1, each inherited from asymptomatic parents. One of the mutations is novel. This is the first described case of a KLF1-null human. The phenotype of severe nonspherocytic hemolytic anemia, jaundice, hepatosplenomegaly, and marked erythroblastosis is more severe than that present in congenital dyserythropoietic anemia type IV as a result of dominant mutations in the second zinc-finger of KLF1. There was a very high level of HbF expression into childhood (>70%), consistent with a key role for KLF1 in human hemoglobin switching. We performed RNA-seq on circulating erythroblasts and found that human KLF1 acts like mouse Klf1 to coordinate expression of many genes required to build a red cell including those encoding globins, cytoskeletal components, AHSP, heme synthesis enzymes, cell-cycle regulators, and blood group antigens. We identify novel KLF1 target genes including KIF23 and KIF11 which are required for proper cytokinesis. We also identify new roles for KLF1 in autophagy, global transcriptional control, and RNA splicing. We suggest loss of KLF1 should be considered in otherwise unexplained cases of severe neonatal NSHA or hydrops fetalis. (Blood. 2015;125(15):2405-2417

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“…43,44 KLF8 knockout mice have normal erythroid parameters. 45 The KLF3/KLF8 double knockout causes embryonic lethality, and greater dysregulation of fetal liver gene expression than either single knockout. 45 The reduced number of E10.5 KLF1-/-KLF2-/-peripheral blood cells stems from a defect in erythroid precursor maintenance and maturation.…”

mentioning

confidence: 99%

“…45 The KLF3/KLF8 double knockout causes embryonic lethality, and greater dysregulation of fetal liver gene expression than either single knockout. 45 The reduced number of E10.5 KLF1-/-KLF2-/-peripheral blood cells stems from a defect in erythroid precursor maintenance and maturation. Primitive erythroid progenitor colonies (EryP-CFC) derived from E8.5 KLF1-/-embryos are similar in frequency but significantly smaller in size than wild-type.…”

mentioning

confidence: 99%

Kruppel-like transcription factors KLF1 and KLF2 have unique and coordinate roles in regulating embryonic erythroid precursor maturation

et al. 2014

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The Krüppel-like transcription factors KLF1 and KLF2 are essential for embryonic erythropoiesis. They can partially compensate for each other during mouse development, and coordinately regulate numerous erythroid genes, including the b-like globins. Simultaneous ablation of KLF1 and KLF2 results in earlier embryonic lethality and severe anemia. In this study, we determine that this anemia is caused by a paucity of blood cells, and exacerbated by diminished b-like globin gene expression. The anemia phenotype is dose-dependent, and, interestingly, can be ameliorated by a single copy of the KLF2, but not the KLF1 gene. The roles of KLF1 and KLF2 in maintaining normal peripheral blood cell numbers and globin mRNA amounts are erythroid cell-specific. Mechanistic studies led to the discovery that KLF2 has an essential function in erythroid precursor maintenance. KLF1 can partially compensate for KLF2 in this role, but is uniquely crucial for erythroid precursor proliferation through its regulation of G1-to S-phase cell cycle transition. A more drastic impairment of primitive erythroid colony formation from embryonic progenitor cells occurs with simultaneous loss of KLF1 and KLF2 than with loss of a single factor. KLF1 and KLF2 coordinately regulate several proliferation-associated genes, including Foxm1. Differential expression of FoxM1, in particular, correlates with the observed KLF1 and KLF2 gene dosage effects on anemia. Furthermore, KLF1 binds to the FoxM1 gene promoter in blood cells. Thus KLF1 and KLF2 coordinately regulate embryonic erythroid precursor maturation through the regulation of multiple homeostasis-associated genes, and KLF2 has a novel and essential role in this process.

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Generation of Mice Deficient in both KLF3/BKLF and KLF8 Reveals a Genetic Interaction and a Role for These Factors in Embryonic Globin Gene Silencing

Cited by 41 publications

References 107 publications

Mutations in Krüppel-like factor 1 cause transfusion-dependent hemolytic anemia and persistence of embryonic globin gene expression

Mutations in Krüppel-like factor 1 cause transfusion-dependent hemolytic anemia and persistence of embryonic globin gene expression

KLF1-null neonates display hydrops fetalis and a deranged erythroid transcriptome

Kruppel-like transcription factors KLF1 and KLF2 have unique and coordinate roles in regulating embryonic erythroid precursor maturation

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