| Molecular Profile |
Indication/Tumor Type |
Response Type |
Relevant Treatment Approaches |
Therapy Name |
Approval Status |
Evidence Type |
Efficacy Evidence |
References |
|
TP53 mutant
|
glioblastoma multiforme
|
sensitive
|
|
Adavosertib
|
Preclinical - Pdx |
Actionable |
In a preclinical study, treatment with MK-1775 decreased CDK1 phosphorylation and reduced tumor growth in patient-derived xenograft models of glioblastoma multiforme that harbor TP53 mutations (PMID: 27196784).
|
27196784
|
|
TP53 mutant
|
triple-receptor negative breast cancer
|
predicted - sensitive
|
|
Carboplatin + Nutlin-3
|
Preclinical - Cell culture |
Actionable |
In a preclinical study, Nutlin-3 and Paraplatin (carboplatin) synergistically inhibited growth in TP53 mutated triple-receptor negative breast cancer cell lines in culture and in cell line xenograft models (PMID: 26494859).
|
26494859
|
|
TP53 mutant
|
fibrous histiocytoma
|
predicted - sensitive
|
|
GDC-0575 + Gemcitabine
|
Preclinical - Pdx |
Actionable |
In a preclinical study, GDC-0575 and Gemzar (gemcitabine) combination treatment inhibited tumor growth, prolonged progression-free survival in patient-derived xenogrft (PDX) models of undifferentiated pleomorphic sarcoma (fibrous histiocytoma) (PMID: 29409053).
|
29409053
|
|
TP53 mutant
|
non-small cell lung carcinoma
|
predicted - sensitive
|
|
Pembrolizumab
|
Phase I |
Actionable |
In a clinical study, a retrospective analysis of a Phase I trial demonstrated non-small cell lung carcinoma (NSCLC) patients harboring either a TP53 mutation (n=15) or KRAS mutation (n=8) had greater progression free survival compared to NSCLC patients harboring wild-type TP53 or KRAS (n=15) (14.5mo vs 14.7mo vs 3.5mo, respectively) when treated with Keytruda (pembrolizumab) (PMID: 28039262).
|
28039262
|
|
TP53 mutant
|
chronic lymphocytic leukemia
|
predicted - sensitive
|
|
Ibrutinib + Venetoclax
|
Phase II |
Actionable |
In a Phase II trial, Imbruvica (ibrutinib) and Venclexta (venetoclax) combination therapy resulted in a response rate of 100% (14/14, 9 complete response, 5 partial response) in relapsed or refractory chronic lymphocytic leukemia (CLL) patients, and a response rate of 100% (16/16, 9 complete response, 7 partial response) in untreated patients with high-risk features including del 17p, TP53 mutations, and del 11q (ASH, 59th Annual Meeting and Exposition, Dec 2017, Abstract 429; NCT02756897).
|
detail...
|
|
TP53 mutant
|
neuroblastoma
|
resistant
|
|
MI-63
|
Preclinical |
Actionable |
In a preclinical study, neuroblastoma cell lines harboring TP53 mutant were resistant to MI-63 mediated growth inhibition (PMID: 21725357).
|
21725357
|
|
TP53 mutant
|
myelodysplastic syndrome
|
not applicable
|
|
N/A
|
Guideline |
Prognostic |
TP53 mutations except P47S and P72R are associated with a poor prognosis in patients with myelodysplastic syndrome (NCCN.org).
|
detail...
|
|
TP53 mutant
|
Advanced Solid Tumor
|
sensitive
|
|
CTX-1
|
Preclinical |
Actionable |
In a preclinical study, CTX-1 induced increased Tp53 protein levels and cell death in human tumor cell lines with mutant Tp53 in culture (PMID: 26883273).
|
26883273
|
|
TP53 mutant
|
colorectal cancer
|
sensitive
|
|
Prodigiosin
|
Preclinical - Cell line xenograft |
Actionable |
In a preclinical study, Prodigiosin inhibited self-renewal of colorectal cancer cell lines harboring TP53 mutations in culture and suppressed tumor growth in cell line xenograft models (PMID: 26759239).
|
26759239
|
|
TP53 mutant
|
colon carcinoma
|
predicted - sensitive
|
|
Camptothecin + CHIR-124
|
Preclinical - Cell culture |
Actionable |
In a preclinical study, the combination of Camptothecin and CHIR-124 demonstrated synergy in TP53-mutant colon carcinoma cell lines in culture, resulting in increased growth inhibition (PMID: 17255282).
|
17255282
|
|
TP53 mutant
|
CLL/SLL
|
sensitive
|
|
Idelalisib + Rituximab
|
Guideline |
Actionable |
Zydelig (idelalisib) combined with Rituxan (rituximab) is indicated in the guidelines for chronic lymphocytic leukemia/small lymphocytic lymphoma patients with a TP53 mutation (NCCN.org).
|
detail...
|
|
TP53 mutant
|
breast carcinoma
|
predicted - sensitive
|
|
Camptothecin + CHIR-124
|
Preclinical - Cell culture |
Actionable |
In a preclinical study, the combination of Camptothecin and CHIR-124 demonstrated synergy in TP53-mutant breast carcinoma cell lines in culture, resulting in increased growth inhibition (PMID: 17255282).
|
17255282
|
|
TP53 mutant
|
colorectal cancer
|
sensitive
|
|
Bevacizumab
|
Phase III |
Actionable |
In a Phase III trial, Avastin (bevacizumab), in combination with chemotherapy, provided a significant survival benefit in patients with colorectal cancers regardless of mutational status in KRAS, BRAF, and TP53 (PMID: 17145525).
|
17145525
|
|
TP53 mutant
|
hypopharynx cancer
|
predicted - sensitive
|
|
unspecified EGFR antibody + unspecified IGF-1R antibody
|
Preclinical - Cell culture |
Actionable |
In a preclinical study, combination of an unspecified EGFR antibody and an unspecified Igf-1r antibody resulted in inhibition of survival in TP53 mutated hypopharyngeal carcinoma cancer cells that developed Erbitux (cetuximab) resistance in culture (PMID: 27196767).
|
27196767
|
|
TP53 mutant
|
medulloblastoma
|
decreased response
|
|
JQ1
|
Preclinical |
Actionable |
In a preclinical study, medulloblastoma cell lines with TP53 mutations had significantly less sensitivity to the BET inhibitor, JQ1, than cell lines carrying wild-type TP53 (PMID: 24231268).
|
24231268
|
|
TP53 mutant
|
triple-receptor negative breast cancer
|
predicted - sensitive
|
|
Doxorubicin + Seliciclib
|
Preclinical - Cell line xenograft |
Actionable |
In a preclinical study, sequential administration of Roscovotine (seliciclib) followed by Adriamycin (doxorubicin) synergistically induced apoptosis in TP53-mutant triple-receptor negative breast cancer cell lines in culture, and inhibited tumor growth, prolonged survival in cell line xenograft models (PMID: 26826118).
|
26826118
|
|
TP53 mutant
|
colorectal cancer
|
sensitive
|
|
PD0166285
|
Preclinical |
Actionable |
In a preclinical study, PD0166285 sensitizes colorectal cancer cells with TP53 mutation to radiation induced cell death (PMID: 11719452).
|
11719452
|
|
TP53 mutant
|
acute myeloid leukemia
|
predicted - sensitive
|
|
Cytarabine + Venetoclax
|
Phase Ib/II |
Actionable |
In a Phase I/II trial, Venclexta (venetoclax) in combination with low-dose cytarabine resulted in complete remission or complete remission with incomplete count recovery in 30% (3/10) of patients with acute myeloid leukemia harboring TP53 mutations who were ineligible for intensive chemotherapy (ASH Annual Meeting, Dec 2018, Abstract 284; NCT02287233).
|
detail...
|
|
TP53 mutant
|
Advanced Solid Tumor
|
sensitive
|
|
Pazopanib + Vorinostat
|
Phase I |
Actionable |
In a Phase I trial, the combination of Votrient (pazopanib) and Zolinza (vorinostat) improved progression-free survival and overall survival in advanced solid tumor patients harboring TP53 hotspot mutations, and resulted in an increased stable disease rate of 45% (5/11), compared to a stable disease rate of 16% (4/25) in patients without detected TP53 mutations (PMID: 25669829).
|
25669829
|
|
TP53 mutant
|
hypopharynx cancer
|
resistant
|
|
unspecified EGFR antibody
|
Preclinical - Cell culture |
Actionable |
In a preclinical study, combination of two unspecified EGFR antibodies targeting nonoverlapping epitopes of Egfr did not inhibit proliferation of Tp53 mutated hypopharyngeal carcinoma cells that developed Erbitux (cetuximab) resistance in culture (PMID: 27196767).
|
27196767
|
|
TP53 mutant
|
glioblastoma multiforme
|
sensitive
|
|
MK-1775 + Radiotherapy
|
Preclinical - Cell line xenograft |
Actionable |
In a preclinical study, the combination of MK-1775 and radiation therapy synergized to inhibit tumor growth in a human glioblastoma multiforme cell line xenograft model harboring mutant TP53 (PMID: 21992793).
|
21992793
|
|
TP53 mutant
|
Advanced Solid Tumor
|
sensitive
|
|
Adavosertib
|
Phase I |
Actionable |
In a retrospective analysis of a Phase I trial, MK-1775 combined with a chemotherapy resulted in a 21% (4/19) response rate in advanced solid tumor patients harboring a TP53 mutation and in those without a TP53 mutation, a 12% (4/33) response rate was observed (PMID: 27601554).
|
27601554
|
|
TP53 mutant
|
breast cancer
|
sensitive
|
|
PK11007
|
Preclinical - Cell culture |
Actionable |
In a preclinical study, TP53-mutated breast cancer cell lines demonstrated increased sensitivity to PK11007 compared to TP53-wild type cells in culture, regardless of Esr1 and Erbb2 (Her2) status (J Clin Oncol 35, 2017 (suppl; abstr e14099)).
|
detail...
|
|
TP53 mutant
|
neuroblastoma
|
resistant
|
|
Nutlin-3a
|
Preclinical |
Actionable |
In a preclinical study, neuroblastoma cell lines harboring TP53 mutant were resistant to nutlin-3 mediated growth inhibition (PMID: 21725357).
|
21725357
|
|
TP53 mutant
|
chronic lymphocytic leukemia
|
predicted - sensitive
|
|
Duvelisib
|
Phase I |
Actionable |
In a Phase I trial, Copiktra (duvelisib) treatment inhibited Akt phosphorylation, resulted in complete response in 2% (1/49), partial response in 53% (26/49), and stable disease in 43% (21/49) of chronic lymphocytic leukemia patients, of which 49% (23/47) carried TP53 mutations (Blood 124 (21): 3334).
|
detail...
|
|
TP53 mutant
|
CLL/SLL
|
sensitive
|
|
Ibrutinib
|
Guideline |
Actionable |
Imbruvica (ibrutinib) is indicated in the guidelines for chronic lymphocytic leukemia/small lymphocytic lymphoma patients with a TP53 mutation (NCCN.org).
|
detail...
|
|
TP53 mutant
|
head and neck squamous cell carcinoma
|
sensitive
|
|
AZD7762 + Cisplatin
|
Preclinical |
Actionable |
In a preclinical study, the treatment of a head and neck squamous cell carcinoma cell line with mutant TP53 (C176F and A161S) with AZD7762, a pan Chk1/2 inhibitor, sensitizes the cells to Platinol (cisplatin) (PMID: 23839309).
|
23839309
|
|
TP53 mutant
|
non-small cell lung carcinoma
|
sensitive
|
|
CEP-8983 + Cisplatin
|
Preclinical |
Actionable |
In a preclinical study, the combination of CEP-8983 and Platinol (cisplatin) worked synergistically to induce cell death in non-small cell lung cancer cell lines in culture, irrespective of TP53 status (PMID: 23428903).
|
23428903
|
|
TP53 mutant
|
ovarian clear cell adenocarcinoma
|
decreased response
|
|
DS-7423
|
Preclinical |
Actionable |
In a preclinical study, ovarian clear cell adenocarcinoma cell lines harboring TP53 mutations demonstrated reduced sensitivity to DS-7423 induced apoptosis in culture compared to TP53 wild-type cells (PMID: 24504419).
|
24504419
|
|
TP53 mutant
|
ovarian cancer
|
predicted - sensitive
|
|
MK-1775 + Carboplatin
|
Phase II |
Actionable |
In a Phase II trial, Paraplatin (carboplatin) and MK-1775 combination treatment resulted in an overall response rate of 43% (9/21), a median progression-free survival of 5.3 months and a median overall survival of 12.6 months in ovarian cancer patients harboring TP53 mutations (PMID: 27998224).
|
27998224
|
|
TP53 mutant
|
colorectal cancer
|
predicted - sensitive
|
|
NSC59984
|
Preclinical - Cell line xenograft |
Actionable |
In a preclinical study, NSC59984 treatment resulted in increased Tp53 signaling and cell death in colorectal cancer cell lines harboring TP53 mutations, and inhibited tumor growth in TP53-mutant cell line colorectal cancer xenograft models (PMID: 26294215).
|
26294215
|
|
TP53 mutant
|
pharynx squamous cell carcinoma
|
sensitive
|
|
AZD6738 + Radiotherapy
|
Preclinical - Cell culture |
Actionable |
In a preclinical study, AZD6738 treatment increased sensitivity to radiotherapy in a pharynx squamous cell carcinoma cell line harboring a TP53 mutation in culture, resulting in a greater decrease in cell survival compared to radiation treatment alone (PMID: 28062704).
|
28062704
|
|
TP53 mutant
|
Advanced Solid Tumor
|
resistant
|
|
AMG 232
|
Preclinical - Cell culture |
Actionable |
In a preclinical study, AMG 232 did not inhibit growth of human tumor cell lines harboring TP53 mutations in culture (PMID: 25567130).
|
25567130
|
|
TP53 mutant
|
neuroblastoma
|
resistant
|
|
GSK2830371
|
Preclinical |
Actionable |
In a preclinical study, neuroblastoma cell lines harboring TP53 mutations were resistant to GSK2830371 induced growth inhibition in culture (PMID: 25658463).
|
25658463
|
|
TP53 mutant
|
essential thrombocythemia
|
not applicable
|
|
N/A
|
Guideline |
Prognostic |
The presence of at least one mutation in either SH2B3, IDH2, U2AF1, SF3B1, EZH2, or TP53 is associated with inferior overall survival in patients with essential thrombocythemia (NCCN.org).
|
detail...
|
|
TP53 mutant
|
essential thrombocythemia
|
not applicable
|
|
N/A
|
Guideline |
Prognostic |
TP53 mutations are associated with inferior leukemia-free survival in patients with essential thrombocythemia (NCCN.org).
|
detail...
|
|
TP53 mutant
|
CLL/SLL
|
sensitive
|
|
Venetoclax
|
Guideline |
Actionable |
Venclexta (venetoclax) is indicated in the guidelines for chronic lymphocytic leukemia/small lymphocytic lymphoma patients with a TP53 mutation (NCCN.org).
|
detail...
|
|
TP53 mutant
|
triple-receptor negative breast cancer
|
predicted - sensitive
|
|
GDC-0425 + Gemcitabine
|
Phase I |
Actionable |
In a Phase I trial, treatment with GDC-0425 followed by Gemzar (gemcitabine) resulted in a partial response in a patient with triple-receptor negative breast cancer harboring a TP53 mutation (PMID: 27815358).
|
27815358
|
|
TP53 mutant
|
colorectal cancer
|
sensitive
|
|
Pazopanib + Vorinostat
|
Phase I |
Actionable |
In a Phase I trial, the combination of Votrient (pazopanib) and Zolinza (vorinostat) resulted in improved progression-free survival and overall survival in metastatic sarcoma and colorectal cancer patients harboring TP53 hotspot mutations, and resulted in a stable disease rate of 83% (5/6), compared to a stable disease rate of 9% (1/11) in patients without detected TP53 mutations (PMID: 25669829).
|
25669829
|
|
TP53 mutant
|
hypopharynx cancer
|
predicted - sensitive
|
|
unspecified EGFR antibody + unspecified ERBB3 antibody
|
Preclinical - Cell culture |
Actionable |
In a preclinical study, combination of an unspecified EGFR antibody and an unspecified Erbb3 (Her3) antibody resulted in inhibition of survival in TP53 mutated hypopharyngeal carcinoma cancer cells that developed Erbitux (cetuximab) resistance in culture (PMID: 27196767).
|
27196767
|
|
TP53 mutant
|
hypopharynx cancer
|
predicted - sensitive
|
|
EGFR antibody + ERBB3 antibody + IGF-1R antibody
|
Preclinical - Cell culture |
Actionable |
In a preclinical study, combination of an unspecified EGFR antibody, an unspecified Erbb3 (Her3) antibody, and an unspecified Igf-1r antibody resulted in potent inhibition of survival in TP53 mutated hypopharyngeal carcinoma cancer cells that developed Erbitux (cetuximab) resistance in culture (PMID: 27196767).
|
27196767
|
|
TP53 mutant
|
sarcoma
|
sensitive
|
|
Pazopanib + Vorinostat
|
Phase I |
Actionable |
In a Phase I trial, the combination of Votrient (pazopanib) and Zolinza (vorinostat) resulted in improved progression-free survival and overall survival in metastatic sarcoma and colorectal cancer patients harboring TP53 hotspot mutations, and resulted in a stable disease rate of 83% (5/6), compared to a stable disease rate of 9% (1/11) in patients without detected TP53 mutations (PMID: 25669829).
|
25669829
|
|
TP53 mutant
|
Advanced Solid Tumor
|
sensitive
|
|
Bevacizumab
|
Clinical Study |
Actionable |
In a clinical study, 106 advanced solid tumor patients harboring a TP53 mutation demonstrated a greater sensitivity to VEGF/VEGFR inhibitors, such as Avastin (bevacizumab), when compared to 82 treated patients harboring TP53 wild-type, resulting in improved rates of SD, PR, and CR, better time-to-treatment failure, and overall survival (PMID: 27466356).
|
27466356
|
|
TP53 mutant
|
Advanced Solid Tumor
|
sensitive
|
|
Bevacizumab
|
Clinical Study |
Actionable |
In a retrospective study, Avastin (bevacizumab) treatment was associated with increased progression-free survival in cancer patients carrying TP53 mutations (PMID: 23670029).
|
23670029
|
|
TP53 mutant
|
ovarian cancer
|
no benefit
|
|
Nutlin-3a
|
Preclinical |
Actionable |
In a preclinical study, treatment with Nutlin-3 had little effect on growth of ovarian cancer cells with TP53 mutations in culture (PMID: 25964101).
|
25964101
|
|
TP53 mutant
|
CLL/SLL
|
sensitive
|
|
GDC-0199 + Rituximab
|
Guideline |
Actionable |
Venclexta (venetoclax) combined with Rituxan (rituximab) is indicated in the guidelines for chronic lymphocytic leukemia/small lymphocytic lymphoma patients with a TP53 mutation (NCCN.org).
|
detail...
|
|
TP53 mutant
|
ovarian serous carcinoma
|
sensitive
|
|
thioureidobutyronitrile
|
Preclinical - Cell culture |
Actionable |
In a preclinical study, Kevetrin (thioureidobutyronitrile) treatment decreased mutant Tp53 level, resulted in apoptosis of ovarian serous carcinoma cells harboring TP53 mutations in culture (Proceedings of the AACR, Vol 58, Apr 2017, abstract # 3221).
|
detail...
|
|
TP53 mutant
|
sarcoma
|
sensitive
|
|
Pazopanib
|
Clinical Study |
Actionable |
In a retrospective study, advanced sarcoma patients with TP53 mutations displayed improved progression-free survival (208 days versus 136 days) relative to patients with wild-type TP53 when treated with Votrient (pazopanib) (PMID: 26646755).
|
26646755
|
|
TP53 mutant
|
glioblastoma multiforme
|
sensitive
|
|
AZD1390
|
Preclinical - Cell culture |
Actionable |
In a preclinical study, TP53 mutant glioblastoma cells demonstrated increased sensitivity to radiosensitization by AZD1390 treatment compared to TP53 wild-type cells in culture (Mol Cancer Ther 2018;17(1 Suppl):Abstract nr A104).
|
detail...
|
|
TP53 mutant
|
osteosarcoma
|
not applicable
|
|
N/A
|
Guideline |
Risk Factor |
Germline mutations in TP53 result in Li-Fraumeni syndrome, which is associated with increased risk of developing osteosarcoma (NCCN.org).
|
detail...
|
|
TP53 mutant
|
sarcoma
|
predicted - sensitive
|
|
GDC-0575 + Gemcitabine
|
Clinical Study |
Actionable |
In a preclinical study, GDC-0575 and Gemzar (gemcitabine) combination treatment resulted in prolonged tumor response in 2 soft tissue sarcoma patients harboring TP53 mutations, and no response in a patient with TP53 wild-type tumor (PMID: 29409053).
|
29409053
|
|
TP53 mutant
|
leukemia
|
decreased response
|
|
RG7112
|
Phase I |
Actionable |
In a Phase I clinical trial, the majority of 19 leukemia patients with identified TP53 mutations did not demonstrate response to treatment with RG7112, with 2 acute myeloid leukemia patients harboring TP53 mutations showing clinical activity, but not improvement, and 1 sCLL/CLL patient achieving stable disease (PMID: 26459177).
|
26459177
|
|
TP53 mutant
|
ovarian cancer
|
sensitive
|
|
Nutlin-3 + Etoposide
|
Preclinical |
Actionable |
In a preclinical study, Nutlin-3 and etoposide worked cooperatively to induce apoptosis in ovarian cancer cell lines with TP53 inactivating mutations in culture (PMID: 25964101).
|
25964101
|
|
TP53 mutant
|
head and neck squamous cell carcinoma
|
predicted - sensitive
|
|
Buparlisib + Paclitaxel
|
Phase II |
Actionable |
In a Phase II (BERIL-1) trial, Buparlisib (BKM120) and Taxol (paclitaxel) combination treatment resulted in improved overall survival (HR=0.52) and prolonged progression-free survival (HR=0.45) in head and neck squamous cell carcinoma patients harboring TP53 mutations compared to TP53 wild-type patients (PMID: 29490986; NCT01852292).
|
29490986
|
|
TP53 mutant
|
tongue squamous cell carcinoma
|
sensitive
|
|
AZD6738 + Radiotherapy
|
Preclinical - Cell culture |
Actionable |
In a preclinical study, AZD6738 treatment increased sensitivity to radiotherapy in a tongue squamous cell carcinoma cell line harboring a TP53 mutation in culture, resulting in a greater decrease in cell survival compared to radiation treatment alone (PMID: 28062704).
|
28062704
|