Primate-restricted KRAB zinc finger proteins and target retrotransposons control gene expression in human neurons

In the first days of embryogenesis, transposable element-embedded regulatory sequences (TEeRS) are silenced by Kruppel-associated box (KRAB) zinc finger proteins (KZFPs). Many TEeRS are subsequently co-opted in transcription networks, but how KZFPs influence this process is largely unknown. We identify ZNF417 and ZNF587 as primate-specific KZFPs repressing HERVK (human endogenous retrovirus K) and SVA (SINE-VNTR-Alu) integrants in human embryonic stem cells (ESCs). Expressed in specific regions of the human developing and adult brain, ZNF417/587 keep controlling TEeRS in ESC-derived neurons and brain organoids, secondarily influencing the differentiation and neurotransmission profile of neurons and preventing the induction of neurotoxic retroviral proteins and an interferon-like response. Thus, evolutionarily recent KZFPs and their TE targets partner up to influence human neuronal differentiation and physiology.

Primate-restricted KRAB zinc finger proteins and target retrotransposons control gene expression in human neurons

Deciphering the molecular events leading to the global restoration of the chromatin landscape during mitotic exit

ISSCR standards for the use of human stem cells in basic research

Statistical learning quantifies transposable element-mediated cis-regulation

Deciphering the molecular events leading to the global restoration of the chromatin landscape during mitotic exit

ISSCR standards for the use of human stem cells in basic research

Statistical learning quantifies transposable element-mediated cis-regulation