Cryptic exon inclusion is a molecular signature of LATE-NC in aging brains

We examined whether TDP-43 regulated cryptic exons accumulate in the hippocampus of neuropathologically confirmed LATE-NC cases. We found that several cryptic RNAs are robustly expressed in LATE-NC cases with or without comorbid ADNC and correlate with pT DP-43 abundance; however, the accumulation of cryptic RNAs is more robust in LATE-NC with comorbid ADNC. Additionally, cryptic RNAs can robustly distinguish LATE-NC from healthy controls and AD cases. These findings expand our current understanding and provide novel potential biomarkers for LATE pat hogenesis.

http://link.springer.com/10.1007/s00401-023-02671-0

Source: Acta Neuropathologica - February 3, 2024 Category: Neurology Source Type: research

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