FAAP24, a Fanconi anemia core complex protein, is crucial for DNA damage repair [3,6]. It forms a stable complex with FANCM, anchoring the FA core complex to chromatin in the repair of DNA interstrand crosslinks, and is involved in the Fanconi anemia pathway [3,5]. This interaction with FANCM also aids in remodeling stalled replication forks to facilitate ATR signaling activation in response to replication stress [2].

Isogenic models for FAAP24 have shown that it promotes ATR-mediated checkpoint activation, especially in response to DNA cross-linking agents [4]. In AML, high FAAP24 expression is associated with poor prognosis and the shaping of an immunosuppressive tumor microenvironment, suggesting it could serve as a prognostic biomarker and play an immunomodulatory role [1].

In conclusion, FAAP24 is essential for DNA damage repair and ATR-mediated checkpoint activation. Its role in AML prognosis and immunomodulation, as revealed through functional studies including gene-related models, provides valuable insights into disease mechanisms, potentially guiding future research and treatment strategies for AML and other related diseases.