Analy­sis of the Chro­matin Acces­si­bil­i­ty Land­scape in Patients with Local­ized Prostate Cancer 

To address this, we pro­filed local­ized PCa from AA and CA men using sin­gle-cell spa­tial ATAC-seq and H3K27ac spa­tial CUT&Tag on prosta­te­c­to­my spec­i­mens from the Cen­ter for Prostate Dis­ease Research/​Walter Reed Nation­al Mil­i­tary Med­ical Cen­ter. Machine learn­ing – based anno­ta­tion (Cell­cano) enabled iden­ti­fi­ca­tion of lin­eage-spe­cif­ic chro­matin states. Fur­ther­more, AA demon­strat­ed sig­nif­i­cant low­er acces­si­ble chro­matin asso­ci­at­ed with CCCTCbind­ing fac­tor (CTCF) which is a crit­i­cal zinc fin­ger pro­tein cru­cial for reg­u­lat­ing gene expres­sion, epi­ge­net­ic marks, and main­tain­ing 3‑dimensional genome structure.

We have val­i­dat­ed this find­ing by CTCF immuno­his­to­chem­istry in an inde­pen­dent TMA that includes 99 patients with dis­tri­b­u­tion of CA and AA prosta­te­c­to­my sam­ples. More­over, inte­gra­tion of H3K27ac pro­fil­ing revealed sev­er­al dif­fer­en­tial­ly reg­u­lat­ed enhancer regions near spe­cif­ic genes across sam­ples. Col­lec­tive­ly, our cur­rent find­ings pro­vide crit­i­cal insights into the diver­gent chro­matin acces­si­bil­i­ty pro­files between AA and CA men with local­ized PCa, which like­ly under­lie dis­tinct tran­scrip­tion­al respons­es that can deter­mine ther­a­peu­tic resis­tance and tumor progression.

These data shed light on the com­plex epige­nom­ic mech­a­nisms dri­ving the group-based vari­a­tions in PCa out­comes and may inform the devel­op­ment bet­ter treat­ment strategies.