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. 2020 Mar 3;2(1):zcaa003. doi: 10.1093/narcan/zcaa003

Table 1.

Overview of therapeutic sensitivity of tumours/tissues with indicated phenotype and CDK12 status

Tissue/tumour CDK12 status Related phenotype Drug sensitivity References
Breast (TNBC) WT HR-proficient CDK12 inhibitors (dinaciclib, SR-4835) + PARP inhibitors (olaparib) or DNA-damaging drugs (platinum-based, doxorubicin, irinotecan) (42,116)
Ovarian (HGSOC) and breast Inactivating mutations; shRNA/siRNA depletion of WT HR deficiency PARP inhibitors, DNA-damaging drugs (10,82,83)
Breast (HER2-positive) Genomic disruption (out-of-frame rearrangements due to breakpoint of HER2 amplicon) HR deficiency PARP inhibitors (108,109)
Metastatic osteosarcoma WT HR-proficient CDK12 inhibitors (dinaciclib, THZ531) (117)
Foreskin fibroblasts siRNA depletion of WT c-MYC overexpression (103)
Neuroblastoma and ovarian WT N-MYC/c-MYC amplification CDK inhibitors (roscovitine, CR8, THZ1) (104,124)
Breast (trastuzumab- resistant/sensitive HER2-positive) Amplified HER2 amplification CDK12 inhibitor (dinaciclib, THZ531) (110)
Hepatocellular carcinoma (sorafenib-treated) WT EGFR/HER3 and PI3K/AKT activation CDK12 inhibitor (THZ531) (126)
Ewing sarcoma WT EWS/FLI expression CDK12 inhibitor (THZ531) + PARP inhibitors (olaparib) (128)
Cancer cell lines (colon, ovarian) siRNA depletion of WT Replication stress CHK1 inhibitors (129)
Prostate (mCRPC) Biallelic loss-of-function mutations Focal tandem duplications, high neoantigen load Immune checkpoint (PD-1) inhibitors (88,94,132)
Ovarian (HGSOC) siRNA depletion of WT BRCA1 deficiency (HR deficiency-independent metabolic reprogramming) Metabolic inhibitors (135)

WT = wild-type CDK12.