Schematic representation of the suggested function of PHF6 in restricting the self-renewal capacity of HSCs (left) and how it can go awry in PHF6-mutant backgrounds (right). Lack of PHF6 could be exploited by oncogenic transcription factors, such as NOTCH1 and TLX3, to promote oncogenesis (bottom).

Schematic representation of the suggested function of PHF6 in restricting the self-renewal capacity of HSCs (left) and how it can go awry in PHF6-mutant backgrounds (right). Lack of PHF6 could be exploited by oncogenic transcription factors, such as NOTCH1 and TLX3, to promote oncogenesis (bottom).

Close Modal
This Feature Is Available To Subscribers Only

or Create an Account

Close Modal
Close Modal