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Do patients with tuberous sclerosis complex have an increased risk for malignancies?

Tuberous Sclerosis Complex (TSC) is generally characterized by the presence of benign tumors, but some patients with malignancies have been reported in the literature. We examined a large Italian TSC population (240 individuals followed from 2001 to 2015, aged 3 months–74 years), assessing the frequ...

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Published in:	American journal of medical genetics. Part A 2016-06, Vol.170A (6), p.1538-1544
Main Authors:	Peron, Angela, Vignoli, Aglaia, La Briola, Francesca, Volpi, Angela, Montanari, Emanuele, Morenghi, Emanuela, Ghelma, Filippo, Bulfamante, Gaetano, Cefalo, Graziella, Canevini, Maria Paola
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Language:	English
Subjects:	Adolescent Adult Age of Onset Aged cancer Child Child, Preschool Female Germ-Line Mutation Humans Infant Male malignancy Middle Aged neoplasia Neoplasms - diagnosis Neoplasms - epidemiology Neoplasms - etiology Neoplasms - mortality Phenotype Population Surveillance Retrospective Studies Risk SEER Program TSC TSC1 TSC2 Tuberous Sclerosis - complications Tuberous Sclerosis - epidemiology Tuberous Sclerosis - genetics Tuberous Sclerosis - therapy tuberous sclerosis complex tumor Young Adult
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creator	Peron, Angela Vignoli, Aglaia La Briola, Francesca Volpi, Angela Montanari, Emanuele Morenghi, Emanuela Ghelma, Filippo Bulfamante, Gaetano Cefalo, Graziella Canevini, Maria Paola
description	Tuberous Sclerosis Complex (TSC) is generally characterized by the presence of benign tumors, but some patients with malignancies have been reported in the literature. We examined a large Italian TSC population (240 individuals followed from 2001 to 2015, aged 3 months–74 years), assessing the frequency of malignancies to determine whether there is an increased risk for cancer in this disorder, and looking for possible features associated with the development of neoplasia. Fifteen patients had malignancies (6.25%); median age at diagnosis was 37.5 years (range of 1.6–58). Five of seven renal tumors were renal cell carcinomas. Eight patients had a non‐renal malignancy (3.3%), but we did not find a more prevalent type of cancer. No patient developed more than one malignancy. The prevalence of all malignant tumors was compatible with the prevalence in the general population (5.6%, 95%CI 2.99−9.31%, vs. 4.4% in Italy). Median age at cancer diagnosis was lower (37.5 years, 95%CI 28.6−44.7, vs. 66.0 years). Two patients (13.3%) died of their cancer, while outcome was favorable in the remaining individuals. Malignant tumors were more frequently diagnosed in patients with mutations in TSC1 when compared to TSC2 and patients with no mutation identified (P = 0.032). Our study demonstrated that TSC patients do not seem to have an increased risk for malignancies besides renal cell carcinoma. However, when cancer develops, age at diagnosis is lower than in the general population, and malignant tumors are more frequently diagnosed in patients with mutations in TSC1. Further studies are needed to confirm these data. ©2016 Wiley Periodicals, Inc.
doi_str_mv	10.1002/ajmg.a.37644
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We examined a large Italian TSC population (240 individuals followed from 2001 to 2015, aged 3 months–74 years), assessing the frequency of malignancies to determine whether there is an increased risk for cancer in this disorder, and looking for possible features associated with the development of neoplasia. Fifteen patients had malignancies (6.25%); median age at diagnosis was 37.5 years (range of 1.6–58). Five of seven renal tumors were renal cell carcinomas. Eight patients had a non‐renal malignancy (3.3%), but we did not find a more prevalent type of cancer. No patient developed more than one malignancy. The prevalence of all malignant tumors was compatible with the prevalence in the general population (5.6%, 95%CI 2.99−9.31%, vs. 4.4% in Italy). Median age at cancer diagnosis was lower (37.5 years, 95%CI 28.6−44.7, vs. 66.0 years). Two patients (13.3%) died of their cancer, while outcome was favorable in the remaining individuals. Malignant tumors were more frequently diagnosed in patients with mutations in TSC1 when compared to TSC2 and patients with no mutation identified (P = 0.032). Our study demonstrated that TSC patients do not seem to have an increased risk for malignancies besides renal cell carcinoma. However, when cancer develops, age at diagnosis is lower than in the general population, and malignant tumors are more frequently diagnosed in patients with mutations in TSC1. 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Part A</title><addtitle>Am. J. Med. Genet</addtitle><description>Tuberous Sclerosis Complex (TSC) is generally characterized by the presence of benign tumors, but some patients with malignancies have been reported in the literature. We examined a large Italian TSC population (240 individuals followed from 2001 to 2015, aged 3 months–74 years), assessing the frequency of malignancies to determine whether there is an increased risk for cancer in this disorder, and looking for possible features associated with the development of neoplasia. Fifteen patients had malignancies (6.25%); median age at diagnosis was 37.5 years (range of 1.6–58). Five of seven renal tumors were renal cell carcinomas. Eight patients had a non‐renal malignancy (3.3%), but we did not find a more prevalent type of cancer. No patient developed more than one malignancy. The prevalence of all malignant tumors was compatible with the prevalence in the general population (5.6%, 95%CI 2.99−9.31%, vs. 4.4% in Italy). Median age at cancer diagnosis was lower (37.5 years, 95%CI 28.6−44.7, vs. 66.0 years). Two patients (13.3%) died of their cancer, while outcome was favorable in the remaining individuals. Malignant tumors were more frequently diagnosed in patients with mutations in TSC1 when compared to TSC2 and patients with no mutation identified (P = 0.032). Our study demonstrated that TSC patients do not seem to have an increased risk for malignancies besides renal cell carcinoma. However, when cancer develops, age at diagnosis is lower than in the general population, and malignant tumors are more frequently diagnosed in patients with mutations in TSC1. 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Genet</addtitle><date>2016-06</date><risdate>2016</risdate><volume>170A</volume><issue>6</issue><spage>1538</spage><epage>1544</epage><pages>1538-1544</pages><issn>1552-4825</issn><eissn>1552-4833</eissn><abstract>Tuberous Sclerosis Complex (TSC) is generally characterized by the presence of benign tumors, but some patients with malignancies have been reported in the literature. We examined a large Italian TSC population (240 individuals followed from 2001 to 2015, aged 3 months–74 years), assessing the frequency of malignancies to determine whether there is an increased risk for cancer in this disorder, and looking for possible features associated with the development of neoplasia. Fifteen patients had malignancies (6.25%); median age at diagnosis was 37.5 years (range of 1.6–58). Five of seven renal tumors were renal cell carcinomas. Eight patients had a non‐renal malignancy (3.3%), but we did not find a more prevalent type of cancer. No patient developed more than one malignancy. The prevalence of all malignant tumors was compatible with the prevalence in the general population (5.6%, 95%CI 2.99−9.31%, vs. 4.4% in Italy). Median age at cancer diagnosis was lower (37.5 years, 95%CI 28.6−44.7, vs. 66.0 years). Two patients (13.3%) died of their cancer, while outcome was favorable in the remaining individuals. Malignant tumors were more frequently diagnosed in patients with mutations in TSC1 when compared to TSC2 and patients with no mutation identified (P = 0.032). Our study demonstrated that TSC patients do not seem to have an increased risk for malignancies besides renal cell carcinoma. However, when cancer develops, age at diagnosis is lower than in the general population, and malignant tumors are more frequently diagnosed in patients with mutations in TSC1. Further studies are needed to confirm these data. ©2016 Wiley Periodicals, Inc.</abstract><cop>United States</cop><pub>Blackwell Publishing Ltd</pub><pmid>27061015</pmid><doi>10.1002/ajmg.a.37644</doi><tpages>7</tpages></addata></record>
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subjects	Adolescent Adult Age of Onset Aged cancer Child Child, Preschool Female Germ-Line Mutation Humans Infant Male malignancy Middle Aged neoplasia Neoplasms - diagnosis Neoplasms - epidemiology Neoplasms - etiology Neoplasms - mortality Phenotype Population Surveillance Retrospective Studies Risk SEER Program TSC TSC1 TSC2 Tuberous Sclerosis - complications Tuberous Sclerosis - epidemiology Tuberous Sclerosis - genetics Tuberous Sclerosis - therapy tuberous sclerosis complex tumor Young Adult
title	Do patients with tuberous sclerosis complex have an increased risk for malignancies?
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