Table 1.
Potentially ''actionable'' phenotypes and supporting evidence
| Actionable phenotype | Therapeutic | Rationale | Molecular characterization |
| Gemcitabine responsive | Gemcitabine | In PC, Phase III trials showed benefit in adjuvant (DFS 13.4 mo vs 6.9 mo) and palliative setting (MS 5.65 vs 4.41)[6,87] | High hENT1, hCNT1, hCNT3 Phase III data suggested that hENT1 correlated with response to Gemcitabine in adjuvant setting in PC[65,88], however this was not shown in the metastatic population[89] |
| Anti-EGFR responsive | Erlotinib, Cetuximab | A Phase III trial showed that Erlotinib plus Gemcitabine had an overall survival benefit (HR = 0.82) compared with Gemcitabine alone in PC[14] Phase III data did not show a difference in OS when Cetuximab was added to Gemcitabine in an unselected population with PC[16] | Classical subtypePC cell lines with a “classical” subtype were shown to be more sensitive to Erlotinib[90] EGFR expression did not correlate with response to Cetuximab in patients with PC[16] |
| Taxane responsive | nab-Paclitaxel | Phase III data showed that the addition of nab-Paclitaxel to Gemcitabine increased PFS (HR = 0.69) and OS (HR = 0.72) in the metastatic PC population[13] | SPARC expression (stromal) A phase I/II study showed that SPARC expression in the stroma correlated with survival[71] |
| 5-FU responsive | 5-Fluorouracil | Small phase III trials showed activity of 5-FU containing regimens in the metastatic population in PC[91,92]5-FU was shown to prolong survival when used in the adjuvant setting in PC (HR = 0.7)[93] | Thymidylate SynthaseHigh intra-tumoural expression was shown to correlate with an increased benefit from 5-FU based chemotherapy in pre-clinical[94] and retrospective patient populations[95] |
| Irinotecan responsive | Irinotecan | In PC, a small effect as monotherapy has been shown in the second-line setting[96], and a significant effect on OS was shown when used as part of FOLFIRINOX (HR = 0.57)[11] | Topoisomerase 1 expressionHigh topo 1 expression was associated with a larger benefit from Irinotecan containing regimens in metastatic colorectal cancer[97] |
| HER2 amplified | Trastuzumab | Has shown activity in HER-2 overexpressing breast and gastric cancers[39,98,99]Phase II trials do not show a benefit of adding Trastuzumab to Gemcitabine in PC (OS = 7 mo), however, no standardised approach to FISH testing was used[41,70] | HER2 amplificationPre-clinical studies suggested that HER2 overexpression predicts a response to Trastuzumab in PC[100] |
| m-TOR responsive | Everolimus, Temsirolimus | A phase III trial of Everolimus in renal cell cancer shows prolongation in PFS (PFS 4 mo vs 1.9 mo)[101]Phase II data showed minimal activity (OS = 4.5 mo) of Everolimus for second line treatment in an unselected population of patients with metastatic PC[102]A case study in a patient with PC and Peutz-Jeghers syndrome (SK11 deficient) responds to Everolimus[103] | P-TEN Deficient, High p-mTOR/p70S6, AKT amplified, STK11/LKB1 deficiency, PI3K mutation Pre clinical studies showed that p-TEN deficient cell lines are sensitive to m-TOR inhibitors[104]Retrospective studies suggested that SK11, p-MTOR, p-70S6, PI3K and AKT can select tumours that will respond to m-TOR inhibitors[103,104-110] |
| VEGF inhibitor responsive | Sunitinib, Bevacizumab | Phase III trial showed no benefit with adding Bevacizumab to Gemcitabine in an unselected population of patients with PC[17]Phase II data showed that maintenance Sunitinib after primary chemotherapy improved 2 yr OS (22.9% vs 7%) in the metastatic PC population[109] | CSF1R up-regulation, High HIF-α expressionIn vitro studies showed CSF-1R up-regulation was associated with response to Sunitinib in AML[110]High HIF-α predicted response to Sunitinib in a retrospective cohort in renal cell cancer[111] |
| DNA damage repair deficient | Platinum; MMC; PARP inhibitor | In vitro work showed that cells with defects in BRCA2 are preferentially sensitive to PARP inhibitors[112]Case reports of PC patients with BRCA2 deficient tumours respond to PARP[113,114]Multiple clinical trials are on-going assessing the effects of PARP inhibition | DDR signature; mutation of DDR genes,BRCA/ATM/PALB2Loss of BRCA1 was associated with sensitivity to DNA damaging agents[115]BRCA2 mutations were associated with improved response to platinum agents[116]In vivo studies showed PALB2 inactivation was a determinant of response to DNA damaging agents in PC[114] |
| SMO inhibitor responsive | Saridegib, Vismodegib | A phase II trial found that Saridegib plus Gemcitabine was no better than Gemcitabine alone in an unselected population of metastatic PC patients (data not published)[117]In vivo studies show SMO inhibitors block metastasis formation in pancreatic cancer[118] | Gli1 and PTCH1 transcript levelsGLI1 mRNA may predict response to SMO inhibitors in pancreatic cancer in vivo[119]High Gli1/PTCH1 transcript levels were correlated with response to SMO inhibitors in CLL[120] |
PC: Pancreatic cancers; EGFR: Epidermal growth factor receptor; VEGF: Vascular endothelial growth factor; DFS: Disease-free survival; OS: Overall survival.