Diagnosis of Li-Fraumeni Syndrome: Differentiating TP53 germline mutations from clonal hematopoiesis: Results of the observational AGO-TR1 trial.
Konstantin Weber-LassallePhilipp HarterJan HaukeCorinna ErnstStefan KommossFrederik MarméNana Weber-LassalleKatharina PrieskeDimo DietrichJulika BordeEsther Pohl-RescignoAlexander ReussBeyhan AtasevenChristoph EngelJulia C StinglRita K SchmutzlerEric HahnenPublished in: Human mutation (2018)
The Li-Fraumeni cancer predisposition syndrome (LFS1) presents with a variety of tumor types and the TP53 gene is covered by most diagnostic cancer gene panels. We demonstrate that deleterious TP53 variants identified in blood-derived DNA of 523 patients with ovarian cancer (AGO-TR1 trial) were not causal for the patients' ovarian cancer in three out of six TP53-positive cases. In three out of six patients, deleterious TP53 mutations were identified with low variant fractions in blood-derived DNA but not in the tumor of the patient seeking advice. The analysis of the TP53 and PPM1D genes, both intimately involved in chemotherapy-induced and/or age-related clonal hematopoiesis (CH), in 523 patients and 1,053 age-matched female control individuals revealed that CH represents a frequent event following chemotherapy, affecting 26 of the 523 patients enrolled (5.0%). Considering that TP53 mutations may arise from chemotherapy-induced CH, our findings help to avoid false-positive genetic diagnoses of LFS1.
Keyphrases
- end stage renal disease
- ejection fraction
- newly diagnosed
- chronic kidney disease
- genome wide
- clinical trial
- prognostic factors
- copy number
- case report
- squamous cell carcinoma
- magnetic resonance
- mental health
- radiation therapy
- dna methylation
- oxidative stress
- room temperature
- young adults
- computed tomography
- ionic liquid
- locally advanced
- phase ii