Medical guidelines for Li–Fraumeni syndrome 2019, version 1.1
Li–Fraumeni syndrome (LFS) is a hereditary tumor that exhibits autosomal dominant inheritance. LFS develops in individuals with a pathogenic germline variant of the cancer-suppressor gene, TP53 (individuals with TP53 pathogenic variant). The number of individuals with TP53 pathogenic variant among t...
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Veröffentlicht in: | International journal of clinical oncology 2021-12, Vol.26 (12), p.2161-2178 |
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Zusammenfassung: | Li–Fraumeni syndrome (LFS) is a hereditary tumor that exhibits autosomal dominant inheritance. LFS develops in individuals with a pathogenic germline variant of the cancer-suppressor gene,
TP53
(individuals with
TP53
pathogenic variant). The number of individuals with
TP53
pathogenic variant among the general population is said to be 1 in 500 to 20,000. Meanwhile, it is found in 1.6% (median value, range of 0–6.7%) of patients with pediatric cancer and 0.2% of adult patients with cancer. LFS is diagnosed by the presence of germline
TP53
pathogenic variants. However, patients can still be diagnosed with LFS even in the absence of a
TP53
pathogenic variant if the familial history of cancers fit the classic LFS diagnostic criteria. It is recommended that
TP53
genetic testing be promptly performed if LFS is suspected. Chompret criteria are widely used for the
TP53
genetic test. However, as there are a certain number of cases of LFS that do not fit the criteria, if LFS is suspected,
TP53
genetic testing should be performed regardless of the criteria. The probability of individuals with
TP53
pathogenic variant developing cancer in their lifetime (penetrance) is 75% for men and almost 100% for women. The LFS core tumors (breast cancer, osteosarcoma, soft tissue sarcoma, brain tumor, and adrenocortical cancer) constitute the majority of cases; however, various types of cancers, such as hematological malignancy, epithelial cancer, and pediatric cancers, such as neuroblastoma, can also develop. Furthermore, approximately half of the cases develop simultaneous or metachronous multiple cancers. The types of
TP53
pathogenic variants and factors that modify the functions of
TP53
have an impact on the clinical presentation, although there are currently no definitive findings. There is currently no cancer preventive agent for individuals with
TP53
pathogenic variant. Surgical treatments, such as risk-reducing bilateral mastectomy warrant further investigation. Theoretically, exposure to radiation could induce the onset of secondary cancer; therefore, imaging and treatments that use radiation should be avoided as much as possible. As a method to follow-up LFS, routine cancer surveillance comprising whole-body MRI scan, brain MRI scan, breast MRI scan, and abdominal ultrasonography (US) should be performed immediately after the diagnosis. However, the effectiveness of this surveillance is unknown, and there are problems, such as adverse events associated with a high rate of |
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ISSN: | 1341-9625 1437-7772 |
DOI: | 10.1007/s10147-021-02011-w |