Your search keyword '"Pitkänen, Esa"' showing total 2 results

1. Systematic search for rare variants in Finnish early-onset colorectal cancer patients.

Author

Tanskanen, Tomas, Gylfe, Alexandra E., Katainen, Riku, Taipale, Minna, Renkonen-Sinisalo, Laura, Järvinen, Heikki, Mecklin, Jukka-Pekka, Böhm, Jan, Kilpivaara, Outi, Pitkänen, Esa, Palin, Kimmo, Vahteristo, Pia, Tuupanen, Sari, and Aaltonen, Lauri A.

Subjects

*AGE of onset, *COLON cancer patients, *HERITABILITY, *COLON cancer diagnosis, *NUCLEOTIDE sequencing, *GENETICS of disease susceptibility, *POPULATION

Abstract

The heritability of colorectal cancer (CRC) is incompletely understood, and the contribution of undiscovered rare variants may be important. In search of rare disease-causing variants, we exome sequenced 22 CRC patients who were diagnosed before the age of 40 years. Exome sequencing data from 95 familial CRC patients were available as a validation set. Cases with known CRC syndromes were excluded. All patients were from Finland, a country known for its genetically homogenous population. We searched for rare nonsynonymous variants with allele frequencies below 0.1% in 3,374 Finnish and 58,112 non-Finnish controls. In addition, homozygous and compound heterozygous variants were studied. No genes with rare loss-of-function variants were present in more than one early-onset CRC patient. Three genes ( ADAMTS4 , CYTL1 , and SYNE1 ) harbored rare loss-of-function variants in both early-onset and familial CRC cases. Five genes with homozygous variants in early-onset CRC cases were found ( MCTP2 , ARHGAP12 , ATM , DONSON , and ROS1 ), including one gene ( MCTP2 ) with a homozygous splice site variant. All discovered homozygous variants were exclusive to one early-onset CRC case. Independent replication is required to associate the discovered variants with CRC. These findings, together with a lack of family history in 19 of 22 (86%) early-onset patients, suggest genetic heterogeneity in unexplained early-onset CRC patients, thus emphasizing the requirement for large sample sizes and careful study designs to elucidate the role of rare variants in CRC susceptibility. [ABSTRACT FROM AUTHOR]

Published

2015

2. Nationwide registry-based analysis of cancer clustering detects strong familial occurrence of Kaposi sarcoma.

Author

Kaasinen E, Aavikko M, Vahteristo P, Patama T, Li Y, Saarinen S, Kilpivaara O, Pitkänen E, Knekt P, Laaksonen M, Artama M, Lehtonen R, Aaltonen LA, and Pukkala E

Subjects

Cluster Analysis, Databases, Factual, Female, Finland epidemiology, Humans, Male, Pedigree, Risk Factors, Sarcoma, Kaposi blood, Sarcoma, Kaposi genetics, Sarcoma, Kaposi pathology, Seroepidemiologic Studies, Skin Neoplasms blood, Skin Neoplasms genetics, Skin Neoplasms pathology, Genetic Predisposition to Disease, Herpesvirus 8, Human isolation & purification, Registries, Sarcoma, Kaposi epidemiology, Skin Neoplasms epidemiology

Abstract

Many cancer predisposition syndromes are rare or have incomplete penetrance, and traditional epidemiological tools are not well suited for their detection. Here we have used an approach that employs the entire population based data in the Finnish Cancer Registry (FCR) for analyzing familial aggregation of all types of cancer, in order to find evidence for previously unrecognized cancer susceptibility conditions. We performed a systematic clustering of 878,593 patients in FCR based on family name at birth, municipality of birth, and tumor type, diagnosed between years 1952 and 2011. We also estimated the familial occurrence of the tumor types using cluster score that reflects the proportion of patients belonging to the most significant clusters compared to all patients in Finland. The clustering effort identified 25,910 birth name-municipality based clusters representing 183 different tumor types characterized by topography and morphology. We produced information about familial occurrence of hundreds of tumor types, and many of the tumor types with high cluster score represented known cancer syndromes. Unexpectedly, Kaposi sarcoma (KS) also produced a very high score (cluster score 1.91, p-value <0.0001). We verified from population records that many of the KS patients forming the clusters were indeed close relatives, and identified one family with five affected individuals in two generations and several families with two first degree relatives. Our approach is unique in enabling systematic examination of a national epidemiological database to derive evidence of aberrant familial aggregation of all tumor types, both common and rare. It allowed effortless identification of families displaying features of both known as well as potentially novel cancer predisposition conditions, including striking familial aggregation of KS. Further work with high-throughput methods should elucidate the molecular basis of the potentially novel predisposition conditions found in this study.

Published

2013