AI Article Synopsis
- HAP1 is a human cell line that's good for studying gene changes and mutations due to its unique genetic makeup, but it's unusually sensitive to the cancer drug camptothecin.
- This sensitivity is linked to a problem with TDP1, an enzyme that helps fix certain DNA issues, specifically due to a mutation that disrupts its function.
- Researchers were able to use CRISPR technology to restore TDP1 in HAP1 cells, creating new cell lines that can be used for deeper studies on how DNA repairs itself in the presence of camptothecin.
Article Abstract
HAP1 is a near-haploid human cell line commonly used for mutagenesis and genome editing studies due to its hemizygous nature. We noticed an unusual hypersensitivity of HAP1 to camptothecin, an antineoplastic drug that stabilizes topoisomerase I cleavage complexes (TOP1ccs). We have attributed this hypersensitivity to a deficiency of TDP1, a key phosphodiesterase involved in resolving abortive TOP1ccs. Through whole-exome sequencing and subsequent restoration of TDP1 protein via CRISPR-Cas9 endogenous genome editing, we demonstrate that TDP1 deficiency and camptothecin hypersensitivity in HAP1 cells are a result of a splice-site mutation (TDP1 c.660-1G > A) that causes exon skipping and TDP1 loss of function. The lack of TDP1 in HAP1 cells should be considered when studying topoisomerase-associated DNA lesions and when generalizing mechanisms of DNA damage repair using HAP1 cells. Finally, we also report the generation of HAP1 STAR clones with restored TDP1 expression and function, which may be useful in further studies to probe cellular phenotypes relating to TOP1cc repair.
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| http://dx.doi.org/10.1093/nar/gkae1163 | DOI Listing |
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