Genome‐wide association study follow‐up identifies cyclin A2 as a regulator of the transition through cytokinesis during terminal erythropoiesis

Ludwig, Leif S.; Cho, Hyunjii; Wakabayashi, Aoi; Ulirsch, Jacob C.; Fleming, Mark D.; Lodish, Harvey F.; Sankaran, Vijay G.

doi:10.1002/ajh.23952

Cited by 16 publications

(17 citation statements)

References 26 publications

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“…Fortunately, advances in both sequencing technology and functional approaches have allowed for the direct study of human erythropoiesis and disorders due to alterations of this process. GWAS coupled with thorough functional follow-up have identified novel roles for BCL11A as an essential HbF silencing factor (Sankaran et al, 2008), CCND3 and CCNA2 as regulators of RBC size and number (Ludwig et al, 2015; Sankaran et al, 2012a), TRIM58 as a regulator of enucleation (Thom et al, 2014), and SMIM1 as a key RBC surface protein encoding the Vel blood antigen (Cvejic et al, 2013). Studies of rare genetic disorders in humans have revealed novel, and sometimes unexpected, findings, such as an erythroid-specific defect due to ribosomal protein haploinsufficiency in Diamond Blackfan anaemia (Ludwig et al, 2014).…”

Section: Model Systems and Organisms Used For Understanding Erythropomentioning

confidence: 99%

Advances in understanding erythropoiesis: evolving perspectives

2016

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Red blood cells (RBCs) are generated from haematopoietic stem and progenitor cells (HSPCs) through the step-wise process of differentiation known as erythropoiesis. In this review, we discuss our current understanding of erythropoiesis and highlight recent advances in this field. During embryonic development, erythropoiesis occurs in three distinct waves comprising first, the yolk sac-derived primitive RBCs, followed sequentially by the erythro-myeloid progenitor (EMP) and HSPC-derived definitive RBCs. Recent work has highlighted the complexity and variability that may exist in the hierarchical arrangement of progenitors responsible for erythropoiesis. Using recently defined cell surface markers, it is now possible to enrich the erythroid progenitors and precursors to a much greater extent than has been possible before. While a great deal of knowledge has been gained on erythropoiesis from model organisms, our knowledge of this process is being refined through human genetic studies. Genes mutated in erythroid disorders can now be identified more rapidly by the use of next-generation sequencing techniques. Genome-wide association studies on erythroid traits in healthy populations have also revealed new modulators of erythropoiesis. All of these recent developments have significant promise not only for increasing our understanding of erythropoiesis, but also for improving our ability to intervene when RBC production is perturbed in disease.

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Section: Model Systems and Organisms Used For Understanding Erythropomentioning

confidence: 99%

Advances in understanding erythropoiesis: evolving perspectives

2016

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“…The defects in enucleation in erythroblasts deficient for cyclin A2 were independently confirmed by a recent in vitro study 16 using fetal liver erythroblast culture system. The knockdown of cyclin A2 in fetal liver erythroblasts in culture using short hairpin RNAs led to significant enucleation defects, 16 similar to phenotypes displayed by A2 KO fetal liver erythroblasts and bone marrow in our study. Nevertheless, while they observed proliferation defects, in our study there are only mild or no effects on proliferation.…”

Section: Discussionmentioning

confidence: 66%

Cyclin A2 regulates erythrocyte morphology and numbers

et al. 2016

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Cyclin A2 is an essential gene for development and in haematopoietic stem cells and therefore its functions in definitive erythropoiesis have not been investigated. We have ablated cyclin A2 in committed erythroid progenitors in vivo using erythropoietin receptor promoter-driven Cre, which revealed its critical role in regulating erythrocyte morphology and numbers. Erythroid-specific cyclin A2 knockout mice are viable but displayed increased mean erythrocyte volume and reduced erythrocyte counts, as well as increased frequency of erythrocytes containing Howell-Jolly bodies. Erythroblasts lacking cyclin A2 displayed defective enucleation, resulting in reduced production of enucleated erythrocytes and increased frequencies of erythrocytes containing nuclear remnants. Deletion of the Cdk inhibitor p27 Kip1 but not Cdk2, ameliorated the erythroid defects resulting from deficiency of cyclin A2, confirming the critical role of cyclin A2/Cdk activity in erythroid development. Loss of cyclin A2 in bone marrow cells in semisolid culture prevented the formation of BFU-E but not CFU-E colonies, uncovering its essential role in BFU-E function. Our data unveils the critical functions of cyclin A2 in regulating mammalian erythropoiesis.

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“…Our focus has been on using insight from GWAS to identify regulatory elements and the genes they affect to gain new insight into hematopoiesis. For example, we identified variants altering the levels of cyclins D3 and A2, which have key roles in regulating the cell divisions that occur in the last stages of erythropoiesis before the cells prepare to enucleate and form mature RBCs (45,46). It should be noted that over 75 loci have been identified as associated with RBC and other blood cell traits (47), suggesting that there may be more opportunities to gain important new insight into regulators of erythropoiesis and hematopoiesis through more systematic studies.…”

Section: Common Variation In Rbc Traits and Erythropoiesismentioning

confidence: 99%

Society for Pediatric Research 2015 Young Investigator Award: genetics of human hematopoiesis—what patients can teach us about blood cell production

Wakabayashi

Sankaran

2015

Pediatr Res

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Blood cell production or hematopoiesis is one of the most well-understood paradigms of cell differentiation in the body. The majority of work on hematopoiesis comes from studies that have primarily been conducted in mice, zebrafish, or other valuable model systems. However, it is clear that such model organisms may not consistently and faithfully mimic what is observed in humans with blood disorders. Moreover, there is significant divergence between species that is increasingly being appreciated at the genomic level. As a result, there is an opportunity to use observations in humans to provide a refined view of hematopoiesis. Here, we discuss vignettes from our work that illustrate how insight from human genetics can improve our understanding of blood cell production and identify promising therapeutic approaches for blood disorders.

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Genome‐wide association study follow‐up identifies cyclin A2 as a regulator of the transition through cytokinesis during terminal erythropoiesis

Cited by 16 publications

References 26 publications

Advances in understanding erythropoiesis: evolving perspectives

Advances in understanding erythropoiesis: evolving perspectives

Cyclin A2 regulates erythrocyte morphology and numbers

Society for Pediatric Research 2015 Young Investigator Award: genetics of human hematopoiesis—what patients can teach us about blood cell production

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