GapNode·arcadia

Lack of reproducible CRISPR knock-in in Ciona

Direct experiments achieving reliable CRISPR knock-in in Ciona embryos have not been reproduced, creating a gap for modeling human disease alleles that require knock-ins (e.g., point mutations, specific amino acid changes).

Confidence
70%
active

Related Inference Chains

Constraints and rationale for modeling human genes in Ciona