chr17:7577539:G>A Detail (hg19) (TP53)
Information
Genome
| Assembly | Position |
|---|---|
| hg19 | chr17:7,577,539-7,577,539 |
| hg38 | chr17:7,674,221-7,674,221 View the variant detail on this assembly version. |
HGVS
| Type | Transcript | Protein |
|---|---|---|
| RefSeq | NM_001126116.1:c.346C>T | NP_001119588.1:p.Arg116Trp |
| NM_001276698.1:c.346C>T | NP_001263627.1:p.Arg116Trp | |
| NM_000546.5:c.742C>T | NP_000537.3:p.Arg248Trp |
Summary
MGeND
| Clinical significance |
Pathogenic
not provided
|
| Variant entry | 205 |
| GWAS entry | |
| Disease area statistics | Show details |
Frequency
| JP | HGVD:[No Data.] |
| ToMMo:[No Data.] | |
| NCBN:[No Data.] | |
| NCBN(Hondo):[No Data.] | |
| NCBN(Ryukyu):[No Data.] | |
| East asia | ExAC:<0.001 |
Prediction
ClinVar
| Clinical Significance |
Pathogenic
|
| Review star |  |
| Show details | |
Disease area statistics
MGeND
| Clinical significance | Last evaluated | Condition | Origin | Submission ID | Submitter | Institute | Citation | Comment | Image |
|---|---|---|---|---|---|---|---|---|---|
|
Pathogenic
|
2020/04/20 | bronchus or lung, unspecified |
not provided
|
MGS000041
(TMGS000094) |
Hitoshi Nakagama | National Cancer Center Japan | |||
|
Pathogenic
|
2020/04/20 | oesophagus, unspecified |
not provided
|
MGS000040
(TMGS000095) |
Hitoshi Nakagama | National Cancer Center Japan | |||
|
Pathogenic
|
2020/04/20 | fundus of stomach |
not provided
|
MGS000040
(TMGS000095) |
Hitoshi Nakagama | National Cancer Center Japan | |||
|
Pathogenic
|
2020/04/20 | pyloric antrum |
not provided
|
MGS000040
(TMGS000095) |
Hitoshi Nakagama | National Cancer Center Japan | |||
|
Pathogenic
|
2020/04/20 | stomach, unspecified |
not provided
|
MGS000040
(TMGS000095) |
Hitoshi Nakagama | National Cancer Center Japan | |||
|
Pathogenic
|
2020/04/20 | caecum |
not provided
|
MGS000040
(TMGS000095) |
Hitoshi Nakagama | National Cancer Center Japan | |||
|
Pathogenic
|
2020/04/20 | ascending colon |
not provided
|
MGS000040
(TMGS000095) |
Hitoshi Nakagama | National Cancer Center Japan | |||
|
Pathogenic
|
2020/04/20 | transverse colon |
not provided
|
MGS000040
(TMGS000095) |
Hitoshi Nakagama | National Cancer Center Japan | |||
|
Pathogenic
|
2020/04/20 | descending colon |
not provided
|
MGS000040
(TMGS000095) |
Hitoshi Nakagama | National Cancer Center Japan | |||
|
Pathogenic
|
2020/04/20 | sigmoid colon |
not provided
|
MGS000040
(TMGS000095) |
Hitoshi Nakagama | National Cancer Center Japan | |||
|
Pathogenic
|
2020/04/20 | colon, unspecified |
not provided
|
MGS000040
(TMGS000095) |
Hitoshi Nakagama | National Cancer Center Japan | |||
|
Pathogenic
|
2020/04/20 | malignant neoplasm of rectosigmoid junction |
not provided
|
MGS000040
(TMGS000095) |
Hitoshi Nakagama | National Cancer Center Japan | |||
|
Pathogenic
|
2020/04/20 | malignant neoplasm of rectum |
not provided
|
MGS000040
(TMGS000095) |
Hitoshi Nakagama | National Cancer Center Japan | |||
|
Pathogenic
|
2020/04/20 | anal canal |
not provided
|
MGS000040
(TMGS000095) |
Hitoshi Nakagama | National Cancer Center Japan | |||
|
Pathogenic
|
2020/04/20 | head of pancreas |
not provided
|
MGS000040
(TMGS000095) |
Hitoshi Nakagama | National Cancer Center Japan | |||
|
Pathogenic
|
2020/04/20 | tail of pancreas |
not provided
|
MGS000040
(TMGS000095) |
Hitoshi Nakagama | National Cancer Center Japan | |||
|
Pathogenic
|
2020/04/20 | ill-defined sites within the digestive system |
not provided
|
MGS000040
(TMGS000095) |
Hitoshi Nakagama | National Cancer Center Japan | |||
|
not provided
|
Myelodysplastic syndromes |
somatic
|
MGS000005
(TMGS000006) |
Keizo Horibe | National Hospital Organization Nagoya Medical Center | ||||
|
not provided
|
Acute myeloblastic leukaemia |
somatic
|
MGS000005
(TMGS000006) |
Keizo Horibe | National Hospital Organization Nagoya Medical Center | ||||
|
not provided
|
Adenocarcinoma of esophagus (disorder) |
unknown
|
MGS000021
(TMGS000080) |
Manabu Muto | Kyoto University | ||||
|
not provided
|
Adenocarcinoma of pancreas |
unknown
|
MGS000021
(TMGS000080) |
Manabu Muto | Kyoto University | ||||
|
Pathogenic
|
Ovary |
somatic
|
MGS000038
(TMGS000091) |
Manabu Muto Ichiro Kinoshita |
Kyoto University Department of Medical Oncology Faculty of Medicine and Graduate School of Medicine Hokkaido University |
||||
|
Pathogenic
|
Colorectal |
somatic
|
MGS000038
(TMGS000091) |
Manabu Muto Ichiro Kinoshita |
Kyoto University Department of Medical Oncology Faculty of Medicine and Graduate School of Medicine Hokkaido University |
||||
|
not provided
|
Carcinoma of colon (disorder) |
unknown
|
MGS000023
(TMGS000082) |
Manabu Muto | Kyoto University | ||||
|
not provided
|
Malignant tumor of rectum (disorder) |
unknown
|
MGS000024
(TMGS000083) |
Manabu Muto | Kyoto University | ||||
|
not provided
|
Primary adenocarcinoma of colon (disorder) |
unknown
|
MGS000025
(TMGS000084) |
Manabu Muto | Kyoto University | ||||
|
not provided
|
Adenocarcinoma of duodenum (disorder) |
unknown
|
MGS000025
(TMGS000084) |
Manabu Muto | Kyoto University | ||||
|
not provided
|
Pancreatic cancer (NET) |
somatic
|
MGS000018
(TMGS000110) |
Hitoshi Nakagama | National Cancer Center Japan |
30742731
|
|||
|
not provided
|
Breast cancer |
somatic
|
MGS000018
(TMGS000110) |
Hitoshi Nakagama | National Cancer Center Japan |
30742731
|
|||
|
not provided
|
Soft tissue sarcoma |
somatic
|
MGS000018
(TMGS000110) |
Hitoshi Nakagama | National Cancer Center Japan |
30742731
|
|||
|
not provided
|
pancreatic cancer |
somatic
|
MGS000018
(TMGS000110) |
Hitoshi Nakagama | National Cancer Center Japan |
30742731
|
|||
|
not provided
|
Thymic carcinoma |
somatic
|
MGS000018
(TMGS000110) |
Hitoshi Nakagama | National Cancer Center Japan |
30742731
|
|||
|
not provided
|
Others (Mast cell tumor) |
somatic
|
MGS000018
(TMGS000110) |
Hitoshi Nakagama | National Cancer Center Japan |
30742731
|
|||
|
not provided
|
other |
somatic
|
MGS000039
(TMGS000092) |
Hitoshi Nakagama | National Cancer Center Japan |
29659903
|
|||
|
not provided
|
lung cancer |
somatic
|
MGS000039
(TMGS000092) |
Hitoshi Nakagama | National Cancer Center Japan |
29659903
|
|||
|
Pathogenic
|
2020/04/20 | middle third of oesophagus |
not provided
|
MGS000042
(TMGS000093) |
Hitoshi Nakagama | National Cancer Center Japan | |||
|
Pathogenic
|
2020/04/20 | oesophagus, unspecified |
not provided
|
MGS000042
(TMGS000093) |
Hitoshi Nakagama | National Cancer Center Japan | |||
|
Pathogenic
|
2020/04/20 | fundus of stomach |
not provided
|
MGS000042
(TMGS000093) |
Hitoshi Nakagama | National Cancer Center Japan | |||
|
Pathogenic
|
2020/04/20 | body of stomach |
not provided
|
MGS000042
(TMGS000093) |
Hitoshi Nakagama | National Cancer Center Japan | |||
|
Pathogenic
|
2020/04/20 | pyloric antrum |
not provided
|
MGS000042
(TMGS000093) |
Hitoshi Nakagama | National Cancer Center Japan | |||
|
Pathogenic
|
2020/04/20 | stomach, unspecified |
not provided
|
MGS000042
(TMGS000093) |
Hitoshi Nakagama | National Cancer Center Japan | |||
|
Pathogenic
|
2020/04/20 | duodenum |
not provided
|
MGS000042
(TMGS000093) |
Hitoshi Nakagama | National Cancer Center Japan | |||
|
Pathogenic
|
2020/04/20 | caecum |
not provided
|
MGS000042
(TMGS000093) |
Hitoshi Nakagama | National Cancer Center Japan | |||
|
Pathogenic
|
2020/04/20 | appendix |
not provided
|
MGS000042
(TMGS000093) |
Hitoshi Nakagama | National Cancer Center Japan | |||
|
Pathogenic
|
2020/04/20 | ascending colon |
not provided
|
MGS000042
(TMGS000093) |
Hitoshi Nakagama | National Cancer Center Japan | |||
|
Pathogenic
|
2020/04/20 | transverse colon |
not provided
|
MGS000042
(TMGS000093) |
Hitoshi Nakagama | National Cancer Center Japan | |||
|
Pathogenic
|
2020/04/20 | descending colon |
not provided
|
MGS000042
(TMGS000093) |
Hitoshi Nakagama | National Cancer Center Japan | |||
|
Pathogenic
|
2020/04/20 | sigmoid colon |
not provided
|
MGS000042
(TMGS000093) |
Hitoshi Nakagama | National Cancer Center Japan | |||
|
Pathogenic
|
2020/04/20 | colon, unspecified |
not provided
|
MGS000042
(TMGS000093) |
Hitoshi Nakagama | National Cancer Center Japan | |||
|
Pathogenic
|
2020/04/20 | malignant neoplasm of rectosigmoid junction |
not provided
|
MGS000042
(TMGS000093) |
Hitoshi Nakagama | National Cancer Center Japan | |||
|
Pathogenic
|
2020/04/20 | malignant neoplasm of rectum |
not provided
|
MGS000042
(TMGS000093) |
Hitoshi Nakagama | National Cancer Center Japan | |||
|
Pathogenic
|
2020/04/20 | anal canal |
not provided
|
MGS000042
(TMGS000093) |
Hitoshi Nakagama | National Cancer Center Japan | |||
|
Pathogenic
|
2020/04/20 | malignant neoplasm of gallbladder |
not provided
|
MGS000042
(TMGS000093) |
Hitoshi Nakagama | National Cancer Center Japan | |||
|
Pathogenic
|
2020/04/20 | ampulla of vater |
not provided
|
MGS000042
(TMGS000093) |
Hitoshi Nakagama | National Cancer Center Japan | |||
|
Pathogenic
|
2020/04/20 | head of pancreas |
not provided
|
MGS000042
(TMGS000093) |
Hitoshi Nakagama | National Cancer Center Japan | |||
|
Pathogenic
|
2020/04/20 | body of pancreas |
not provided
|
MGS000042
(TMGS000093) |
Hitoshi Nakagama | National Cancer Center Japan | |||
|
Pathogenic
|
2020/04/20 | tail of pancreas |
not provided
|
MGS000042
(TMGS000093) |
Hitoshi Nakagama | National Cancer Center Japan | |||
|
Pathogenic
|
2020/04/20 | ill-defined sites within the digestive system |
not provided
|
MGS000042
(TMGS000093) |
Hitoshi Nakagama | National Cancer Center Japan | |||
|
Pathogenic
|
2020/04/20 | bronchus or lung, unspecified |
not provided
|
MGS000042
(TMGS000093) |
Hitoshi Nakagama | National Cancer Center Japan | |||
|
Pathogenic
|
2020/04/20 | middle third of oesophagus |
not provided
|
MGS000041
(TMGS000094) |
Hitoshi Nakagama | National Cancer Center Japan | |||
|
Pathogenic
|
2020/04/20 | fundus of stomach |
not provided
|
MGS000041
(TMGS000094) |
Hitoshi Nakagama | National Cancer Center Japan | |||
|
Pathogenic
|
2020/04/20 | pyloric antrum |
not provided
|
MGS000041
(TMGS000094) |
Hitoshi Nakagama | National Cancer Center Japan | |||
|
Pathogenic
|
2020/04/20 | stomach, unspecified |
not provided
|
MGS000041
(TMGS000094) |
Hitoshi Nakagama | National Cancer Center Japan | |||
|
Pathogenic
|
2020/04/20 | ileum |
not provided
|
MGS000041
(TMGS000094) |
Hitoshi Nakagama | National Cancer Center Japan | |||
|
Pathogenic
|
2020/04/20 | caecum |
not provided
|
MGS000041
(TMGS000094) |
Hitoshi Nakagama | National Cancer Center Japan | |||
|
Pathogenic
|
2020/04/20 | descending colon |
not provided
|
MGS000041
(TMGS000094) |
Hitoshi Nakagama | National Cancer Center Japan | |||
|
Pathogenic
|
2020/04/20 | colon, unspecified |
not provided
|
MGS000041
(TMGS000094) |
Hitoshi Nakagama | National Cancer Center Japan | |||
|
Pathogenic
|
2020/04/20 | malignant neoplasm of rectum |
not provided
|
MGS000041
(TMGS000094) |
Hitoshi Nakagama | National Cancer Center Japan | |||
|
Pathogenic
|
2020/04/20 | head of pancreas |
not provided
|
MGS000041
(TMGS000094) |
Hitoshi Nakagama | National Cancer Center Japan | |||
|
Pathogenic
|
2020/04/20 | ill-defined sites within the digestive system |
not provided
|
MGS000041
(TMGS000094) |
Hitoshi Nakagama | National Cancer Center Japan |
ClinVar
| Clinical significance | Last evaluated | Review status | Condition | Origin | Links |
|---|---|---|---|---|---|
|
Pathogenic
|
2023-10-13 | criteria provided, multiple submitters, no conflicts | Li-Fraumeni syndrome 1 |
unknown
germline
|
Detail |
|
Pathogenic
|
2023-12-12 | criteria provided, multiple submitters, no conflicts | Hereditary cancer-predisposing syndrome |
germline
|
Detail |
|
Pathogenic
|
2019-08-28 | reviewed by expert panel | Li-Fraumeni syndrome |
unknown
germline
|
Detail |
|
Pathogenic
|
2022-05-11 | criteria provided, multiple submitters, no conflicts | not provided |
unknown
germline
|
Detail |
Likely pathogenic
|
2016-05-31 | no assertion criteria provided | acute myeloid leukemia |
somatic
|
Detail |
|
Likely pathogenic
|
2016-05-31 | no assertion criteria provided | lung adenocarcinoma |
somatic
|
Detail |
|
Likely pathogenic
|
2016-05-31 | no assertion criteria provided | glioblastoma |
somatic
|
Detail |
|
Likely pathogenic
|
2016-05-31 | no assertion criteria provided | Small cell lung carcinoma |
somatic
|
Detail |
|
Likely pathogenic
|
2016-05-31 | no assertion criteria provided | Squamous cell carcinoma of the head and neck |
somatic
|
Detail |
|
Likely pathogenic
|
2016-05-31 | no assertion criteria provided | B-cell chronic lymphocytic leukemia |
somatic
|
Detail |
|
Likely pathogenic
|
2016-05-31 | no assertion criteria provided |
somatic
|
Detail | |
|
Likely pathogenic
|
2016-05-31 | no assertion criteria provided | ovarian serous cystadenocarcinoma |
somatic
|
Detail |
|
Likely pathogenic
|
2016-05-31 | no assertion criteria provided | myelodysplastic syndrome |
somatic
|
Detail |
|
Likely pathogenic
|
2016-05-31 | no assertion criteria provided | prostate adenocarcinoma |
somatic
|
Detail |
|
Likely pathogenic
|
2016-05-31 | no assertion criteria provided | Breast neoplasm |
somatic
|
Detail |
|
Likely pathogenic
|
2016-05-31 | no assertion criteria provided | Carcinoma of esophagus |
somatic
|
Detail |
|
Likely pathogenic
|
2016-05-31 | no assertion criteria provided | gastric adenocarcinoma |
somatic
|
Detail |
|
Likely pathogenic
|
2016-05-31 | no assertion criteria provided | multiple myeloma |
somatic
|
Detail |
|
Likely pathogenic
|
2016-05-31 | no assertion criteria provided | uterine carcinosarcoma |
somatic
|
Detail |
|
Likely pathogenic
|
2016-05-31 | no assertion criteria provided | Neoplasm of brain |
somatic
|
Detail |
|
Likely pathogenic
|
2016-05-31 | no assertion criteria provided | Squamous cell lung carcinoma |
somatic
|
Detail |
|
Likely pathogenic
|
2016-05-31 | no assertion criteria provided | hepatocellular carcinoma |
somatic
|
Detail |
|
Likely pathogenic
|
2016-05-31 | no assertion criteria provided |
somatic
|
Detail | |
|
Likely pathogenic
|
2015-07-14 | no assertion criteria provided | Neoplasm |
somatic
|
Detail |
|
Likely pathogenic
|
2016-05-31 | no assertion criteria provided | Neoplasm of the large intestine |
somatic
|
Detail |
|
Likely pathogenic
|
2016-05-31 | no assertion criteria provided | medulloblastoma |
somatic
|
Detail |
|
Likely pathogenic
|
2016-05-31 | no assertion criteria provided | Malignant neoplasm of body of uterus |
somatic
|
Detail |
|
Likely pathogenic
|
2016-05-31 | no assertion criteria provided |
somatic
|
Detail | |
|
Likely pathogenic
|
2016-05-31 | no assertion criteria provided | Malignant melanoma of skin |
somatic
|
Detail |
|
Likely pathogenic
|
2016-05-31 | no assertion criteria provided | pancreatic adenocarcinoma |
somatic
|
Detail |
|
Pathogenic
|
criteria provided, single submitter | Pectus excavatum,acute myeloid leukemia,Cognitive impairment |
germline
|
Detail | |
|
Pathogenic
|
criteria provided, single submitter | Pectus excavatum,acute myeloid leukemia,Cognitive impairment |
germline
|
Detail | |
|
Pathogenic
|
criteria provided, single submitter | Pectus excavatum,acute myeloid leukemia,Cognitive impairment |
germline
|
Detail | |
|
Pathogenic
Likely pathogenic
|
2021-03-19 | no assertion criteria provided | Neoplasm of ovary |
somatic
|
Detail |
|
Pathogenic
|
2019-04-30 | no assertion criteria provided | Lip and oral cavity carcinoma |
somatic
|
Detail |
|
Pathogenic
|
2020-12-22 | no assertion criteria provided | choroid plexus carcinoma |
germline
|
Detail |
Uncertain significance
|
2020-10-30 | no assertion criteria provided | gallbladder cancer |
somatic
|
Detail |
|
Pathogenic
|
2022-05-10 | no assertion criteria provided | congenital fibrosarcoma |
somatic
|
Detail |
|
Pathogenic
|
2021-09-07 | criteria provided, single submitter | Breast and/or ovarian cancer |
germline
|
Detail |
|
Pathogenic
|
2021-07-01 | no assertion criteria provided | Gastric cancer |
germline
|
Detail |
|
Pathogenic
|
2023-07-25 | no assertion criteria provided | Malignant lymphoma, large B-cell, diffuse |
somatic
|
Detail |
|
Pathogenic
|
2023-09-27 | criteria provided, single submitter | Adrenocortical carcinoma, hereditary |
unknown
|
Detail |
CIViC
DisGeNET
| Score | Disease name | Description | Source | Pubmed | Links |
|---|---|---|---|---|---|
| 0.080 | Carcinoma of lung | Mutant p53 R248Q but not R248W enhances in vitro invasiveness of human lung canc... | BeFree | 21187651 | Detail |
| 0.441 | Li-Fraumeni syndrome 1 | NA | CLINVAR | Detail | |
| 0.160 | Malignant neoplasm of lung | Mutant p53 R248Q but not R248W enhances in vitro invasiveness of human lung canc... | BeFree | 21187651 | Detail |
| 0.122 | Neoplastic Syndromes, Hereditary | NA | CLINVAR | Detail | |
| 0.369 | Li-Fraumeni syndrome | NA | CLINVAR | Detail | |
| 0.157 | pancreatic carcinoma | Using the whole-cell recording mode of the patch-clamp technique, functional ion... | BeFree | 14978241 | Detail |
| 0.012 | Tumors of Adrenal Cortex | Composite adrenal anaplastic neuroblastoma and virilizing adrenocortical tumor w... | BeFree | 17427234 | Detail |
| 0.007 | Lichen Sclerosus et Atrophicus | In matched samples, immunohistochemistry evaluation of p53 protein expression re... | BeFree | 17554370 | Detail |
| 0.067 | colon carcinoma | To elucidate whether and how mutant p53 acquires its gain-of-function, mutant p5... | BeFree | 18701504 | Detail |
| 0.369 | Li-Fraumeni syndrome | Here, we report a family with LFS harboring a germline TP53 mutation (R248W) loc... | BeFree | 19378321 | Detail |
| 0.002 | pancreatic carcinoma | Using the whole-cell recording mode of the patch-clamp technique, functional ion... | BeFree | 14978241 | Detail |
| 0.369 | Li-Fraumeni syndrome | We report a patient with composite neuroblastoma (NB), adrenocortical tumor (ACT... | BeFree | 17427234 | Detail |
| 0.001 | Squamous cell carcinoma of pharynx | Using short hairpin RNA against p53, transient ectopic expression of wild-type p... | BeFree | 21308745 | Detail |
| <0.001 | Glioma | Overexpression of the paradigmatic p53 mutants p53(R175H), p53(R248W) and p53(R2... | BeFree | 18202704 | Detail |
| 0.039 | Malignant neoplasm of pancreas | Using the whole-cell recording mode of the patch-clamp technique, functional ion... | BeFree | 14978241 | Detail |
| 0.002 | Malignant neoplasm of pancreas | Using the whole-cell recording mode of the patch-clamp technique, functional ion... | BeFree | 14978241 | Detail |
| <0.001 | Anaplastic thyroid carcinoma | Adoptive overexpression of wild-type p53, but not of its inactive (R248W and R27... | BeFree | 15899946 | Detail |
| 0.059 | Malignant tumor of colon | To elucidate whether and how mutant p53 acquires its gain-of-function, mutant p5... | BeFree | 18701504 | Detail |
| 0.127 | neuroblastoma | Composite adrenal anaplastic neuroblastoma and virilizing adrenocortical tumor w... | BeFree | 17427234 | Detail |
| 0.037 | Central neuroblastoma | Composite adrenal anaplastic neuroblastoma and virilizing adrenocortical tumor w... | BeFree | 17427234 | Detail |
Annotation
Annotations
| Descrption | Source | Links |
|---|---|---|
| In breast cancer patients harboring R248W mutation, the prognosis is worse than any other hotspot TP... | CIViC Evidence | Detail |
| Subset of 58 cancer cell lines with unaltered TP53 is sensitive to MDM2 Inhibitor AMGMDS3. None of 1... | CIViC Evidence | Detail |
| NM_000546.6(TP53):c.742C>T (p.Arg248Trp) AND Li-Fraumeni syndrome 1 | ClinVar | Detail |
| NM_000546.6(TP53):c.742C>T (p.Arg248Trp) AND Hereditary cancer-predisposing syndrome | ClinVar | Detail |
| NM_000546.6(TP53):c.742C>T (p.Arg248Trp) AND Li-Fraumeni syndrome | ClinVar | Detail |
| NM_000546.6(TP53):c.742C>T (p.Arg248Trp) AND not provided | ClinVar | Detail |
| NM_000546.6(TP53):c.742C>T (p.Arg248Trp) AND Acute myeloid leukemia | ClinVar | Detail |
| NM_000546.6(TP53):c.742C>T (p.Arg248Trp) AND Lung adenocarcinoma | ClinVar | Detail |
| NM_000546.6(TP53):c.742C>T (p.Arg248Trp) AND Glioblastoma | ClinVar | Detail |
| NM_000546.6(TP53):c.742C>T (p.Arg248Trp) AND Small cell lung carcinoma | ClinVar | Detail |
| NM_000546.6(TP53):c.742C>T (p.Arg248Trp) AND Squamous cell carcinoma of the head and neck | ClinVar | Detail |
| NM_000546.6(TP53):c.742C>T (p.Arg248Trp) AND B-cell chronic lymphocytic leukemia | ClinVar | Detail |
| NM_000546.6(TP53):c.742C>T (p.Arg248Trp) AND Brainstem glioma | ClinVar | Detail |
| NM_000546.6(TP53):c.742C>T (p.Arg248Trp) AND Ovarian serous cystadenocarcinoma | ClinVar | Detail |
| NM_000546.6(TP53):c.742C>T (p.Arg248Trp) AND Myelodysplastic syndrome | ClinVar | Detail |
| NM_000546.6(TP53):c.742C>T (p.Arg248Trp) AND Prostate adenocarcinoma | ClinVar | Detail |
| NM_000546.6(TP53):c.742C>T (p.Arg248Trp) AND Breast neoplasm | ClinVar | Detail |
| NM_000546.6(TP53):c.742C>T (p.Arg248Trp) AND Carcinoma of esophagus | ClinVar | Detail |
| NM_000546.6(TP53):c.742C>T (p.Arg248Trp) AND Gastric adenocarcinoma | ClinVar | Detail |
| NM_000546.6(TP53):c.742C>T (p.Arg248Trp) AND Multiple myeloma | ClinVar | Detail |
| NM_000546.6(TP53):c.742C>T (p.Arg248Trp) AND Uterine carcinosarcoma | ClinVar | Detail |
| NM_000546.6(TP53):c.742C>T (p.Arg248Trp) AND Neoplasm of brain | ClinVar | Detail |
| NM_000546.6(TP53):c.742C>T (p.Arg248Trp) AND Squamous cell lung carcinoma | ClinVar | Detail |
| NM_000546.6(TP53):c.742C>T (p.Arg248Trp) AND Hepatocellular carcinoma | ClinVar | Detail |
| NM_000546.6(TP53):c.742C>T (p.Arg248Trp) AND Transitional cell carcinoma of the bladder | ClinVar | Detail |
| NM_000546.6(TP53):c.742C>T (p.Arg248Trp) AND Neoplasm | ClinVar | Detail |
| NM_000546.6(TP53):c.742C>T (p.Arg248Trp) AND Neoplasm of the large intestine | ClinVar | Detail |
| NM_000546.6(TP53):c.742C>T (p.Arg248Trp) AND Medulloblastoma | ClinVar | Detail |
| NM_000546.6(TP53):c.742C>T (p.Arg248Trp) AND Malignant neoplasm of body of uterus | ClinVar | Detail |
| NM_000546.6(TP53):c.742C>T (p.Arg248Trp) AND Squamous cell carcinoma of the skin | ClinVar | Detail |
| NM_000546.6(TP53):c.742C>T (p.Arg248Trp) AND Malignant melanoma of skin | ClinVar | Detail |
| NM_000546.6(TP53):c.742C>T (p.Arg248Trp) AND Pancreatic adenocarcinoma | ClinVar | Detail |
| NM_000546.6(TP53):c.742C>T (p.Arg248Trp) AND multiple conditions | ClinVar | Detail |
| NM_000546.6(TP53):c.742C>T (p.Arg248Trp) AND multiple conditions | ClinVar | Detail |
| NM_000546.6(TP53):c.742C>T (p.Arg248Trp) AND multiple conditions | ClinVar | Detail |
| NM_000546.6(TP53):c.742C>T (p.Arg248Trp) AND Neoplasm of ovary | ClinVar | Detail |
| NM_000546.6(TP53):c.742C>T (p.Arg248Trp) AND Lip and oral cavity carcinoma | ClinVar | Detail |
| NM_000546.6(TP53):c.742C>T (p.Arg248Trp) AND Choroid plexus carcinoma | ClinVar | Detail |
| NM_000546.6(TP53):c.742C>T (p.Arg248Trp) AND Gallbladder cancer | ClinVar | Detail |
| NM_000546.6(TP53):c.742C>T (p.Arg248Trp) AND Congenital fibrosarcoma | ClinVar | Detail |
| NM_000546.6(TP53):c.742C>T (p.Arg248Trp) AND Breast and/or ovarian cancer | ClinVar | Detail |
| NM_000546.6(TP53):c.742C>T (p.Arg248Trp) AND Gastric cancer | ClinVar | Detail |
| NM_000546.6(TP53):c.742C>T (p.Arg248Trp) AND Malignant lymphoma, large B-cell, diffuse | ClinVar | Detail |
| NM_000546.6(TP53):c.742C>T (p.Arg248Trp) AND Adrenocortical carcinoma, hereditary | ClinVar | Detail |
| Mutant p53 R248Q but not R248W enhances in vitro invasiveness of human lung cancer NCI-H1299 cells. | DisGeNET | Detail |
| NA | DisGeNET | Detail |
| Mutant p53 R248Q but not R248W enhances in vitro invasiveness of human lung cancer NCI-H1299 cells. | DisGeNET | Detail |
| NA | DisGeNET | Detail |
| NA | DisGeNET | Detail |
| Using the whole-cell recording mode of the patch-clamp technique, functional ion channels were elect... | DisGeNET | Detail |
| Composite adrenal anaplastic neuroblastoma and virilizing adrenocortical tumor with germline TP53 R2... | DisGeNET | Detail |
| In matched samples, immunohistochemistry evaluation of p53 protein expression revealed the presence ... | DisGeNET | Detail |
| To elucidate whether and how mutant p53 acquires its gain-of-function, mutant p53 is inducibly knock... | DisGeNET | Detail |
| Here, we report a family with LFS harboring a germline TP53 mutation (R248W) located in the function... | DisGeNET | Detail |
| Using the whole-cell recording mode of the patch-clamp technique, functional ion channels were elect... | DisGeNET | Detail |
| We report a patient with composite neuroblastoma (NB), adrenocortical tumor (ACT), and Li-Fraumeni s... | DisGeNET | Detail |
| Using short hairpin RNA against p53, transient ectopic expression of wild-type p53 or mutant p53 (R2... | DisGeNET | Detail |
| Overexpression of the paradigmatic p53 mutants p53(R175H), p53(R248W) and p53(R273H) in the p53 null... | DisGeNET | Detail |
| Using the whole-cell recording mode of the patch-clamp technique, functional ion channels were elect... | DisGeNET | Detail |
| Using the whole-cell recording mode of the patch-clamp technique, functional ion channels were elect... | DisGeNET | Detail |
| Adoptive overexpression of wild-type p53, but not of its inactive (R248W and R273H) mutants, strongl... | DisGeNET | Detail |
| To elucidate whether and how mutant p53 acquires its gain-of-function, mutant p53 is inducibly knock... | DisGeNET | Detail |
| Composite adrenal anaplastic neuroblastoma and virilizing adrenocortical tumor with germline TP53 R2... | DisGeNET | Detail |
| Composite adrenal anaplastic neuroblastoma and virilizing adrenocortical tumor with germline TP53 R2... | DisGeNET | Detail |
Overlapped Transcript Coordinates
| Gene | Transcript ID | Exon Number | Chromosome | Start | Stop | Type | Amino Mutation | Transcript Position | Links |
|---|
Overlapped Transcript
| Gene | Transcript ID | Chromosome | Start | Stop | Links |
|---|
- Gene
- -
- dbSNP
- rs121912651 dbSNP
- Genome
- hg19
- Position
- chr17:7,577,539-7,577,539
- Variant Type
- snv
- Reference Allele
- G
- Alternative Allele
- A
- East Asian Chromosome Counts (ExAC)
- 8652
- East Asian Allele Counts (ExAC)
- 0
- East Asian Heterozygous Counts (ExAC)
- 0
- East Asian Homozygous Counts (ExAC)
- 0
- East Asian Allele Frequency (ExAC)
- 0.0
- Chromosome Counts in All Race (ExAC)
- 121366
- Allele Counts in All Race (ExAC)
- 1
- Heterozygous Counts in All Race (ExAC)
- 1
- Homozygous Counts in All Race (ExAC)
- 0
- Allele Frequency in All Race (ExAC)
- 8.239539904091756E-6
- Variant (CIViC) (CIViC Variant)
- R248W
- Transcript 1 (CIViC Variant)
- ENST00000269305.4
- Variant URL (CIViC Variant)
- https://civic.genome.wustl.edu/links/variants/118
- Summary (CIViC Variant)
- While loss-of-function events in TP53 are very common in cancer, the R248 variants seem not only to result in loss of tumor-suppression, but also act as a gain-of-function mutation that can promote tumorigenesis in mouse models. This mutant is also more responsive to treatment with doxorubicin than its wild-type counterparts. While the prognostic impact of individual TP53 mutations is influenced by the cohort being studied, R248 mutations have been shown to confer worse overall survival.
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