HAEM5:B-lymphoblastic leukaemia/lymphoma with hypodiploidy: Difference between revisions
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|No established significance | |No established significance | ||
|No (NCCN) | |No (NCCN) | ||
|Approximately 50% of children with low-hypodiploid B-ALL/LBL carry germline ''TP53'' variants associated with Li–Fraumeni syndrome, | |These alterations correlate with low-hypodiploid ALL (32–39 chromosomes) and poorer clinical outcomes<ref name=":2" />. Approximately 50% of children with low-hypodiploid B-ALL/LBL carry germline ''TP53'' variants associated with Li–Fraumeni syndrome. Accordingly, genetic counseling is recommended for children with low-hypodiploid B-ALL carrying ''TP53'' mutations, and their relatives<ref name=":17" />. | ||
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==Familial Forms== | ==Familial Forms== | ||
In Low hypodiploid (LH), several studies have not only identified a high percentage of pediatric patients with ''TP53'' mutations, but close to half displayed germline mutations, suggesting that LH ALL is a manifestation of Li-Fraumeni syndrome in children<ref name=":2" /><ref name=":10" /><ref>{{Cite journal|last=Comeaux|first=Evan Q.|last2=Mullighan|first2=Charles G.|date=2017-03-01|title=TP53 Mutations in Hypodiploid Acute Lymphoblastic Leukemia|url=https://pubmed.ncbi.nlm.nih.gov/28003275|journal=Cold Spring Harbor Perspectives in Medicine|volume=7|issue=3|pages=a026286|doi=10.1101/cshperspect.a026286|issn=2157-1422|pmc=5334249|pmid=28003275}}</ref>. | In Low hypodiploid (LH), several studies have not only identified a high percentage of pediatric patients with ''TP53'' mutations, but close to half displayed germline mutations, suggesting that LH ALL is a manifestation of Li-Fraumeni syndrome in children<ref name=":2" /><ref name=":10" /><ref name=":17">{{Cite journal|last=Comeaux|first=Evan Q.|last2=Mullighan|first2=Charles G.|date=2017-03-01|title=TP53 Mutations in Hypodiploid Acute Lymphoblastic Leukemia|url=https://pubmed.ncbi.nlm.nih.gov/28003275|journal=Cold Spring Harbor Perspectives in Medicine|volume=7|issue=3|pages=a026286|doi=10.1101/cshperspect.a026286|issn=2157-1422|pmc=5334249|pmid=28003275}}</ref>. | ||
Adults also showed a high incidence of ''TP53'' mutations, but these mutations appear to be somatic in origin. In NH, mutations of genes of receptor tyrosine kinase (RTK) pathway, Ras signaling, ''IKZF3'' (17q21.1) and histone clusters, but mutations of ''IZFK2'', ''RB1'', or ''TP53'' were rare. | Adults also showed a high incidence of ''TP53'' mutations, but these mutations appear to be somatic in origin. In NH, mutations of genes of receptor tyrosine kinase (RTK) pathway, Ras signaling, ''IKZF3'' (17q21.1) and histone clusters, but mutations of ''IZFK2'', ''RB1'', or ''TP53'' were rare. | ||