Critical POU domain residues confer Oct4 uniqueness in somatic cell reprogramming
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Changing POU dimerization preferences converts Oct6 into a pluripotency inducer
Changing POU dimerization preferences converts Oct6 into a pluripotency inducer. - Abstract - Europe PMC
An Overview on the Complexity of OCT4: at the Level of DNA, RNA and Protein
A Late Transition in Somatic Cell Reprogramming Requires Regulators Distinct from the Pluripotency Network - ScienceDirect
Critical POU domain residues confer Oct4 uniqueness in somatic cell reprogramming
The roles of the reprogramming factors Oct4, Sox2 and Klf4 in resetting the somatic cell epigenome during induced pluripotent stem cell generation, Genome Biology
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Liquid condensation of reprogramming factor KLF4 with DNA provides a mechanism for chromatin organization
Kap1 regulates the self-renewal of embryonic stem cells and cellular reprogramming by modulating Oct4 protein stability
Evolutionary Origin of Vertebrate OCT4/POU5 Functions in Supporting Pluripotency
Do all roads lead to Oct4? The emerging concepts of induced pluripotency: Trends in Cell Biology
Biomedicines, Free Full-Text
PDF) Critical POU domain residues confer Oct4 uniqueness in somatic cell reprogramming
Proteomic Analysis of Mouse Oocytes Identifies PRMT7 as a Reprogramming Factor that Replaces SOX2 in the Induction of Pluripotent Stem Cells
A unique Oct4 interface is crucial for reprogramming to pluripotency
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