| dc.contributor.author | Rohlin, Anna | |
| dc.date.accessioned | 2015-01-07T10:25:29Z | |
| dc.date.available | 2015-01-07T10:25:29Z | |
| dc.date.issued | 2015-01-07 | |
| dc.identifier.isbn | 978-91-628-9213-5 | |
| dc.identifier.isbn | 978-91-628-9210-4 | |
| dc.identifier.uri | http://hdl.handle.net/2077/37108 | |
| dc.description.abstract | Hereditary factors are thought to play are role in 20-30% of all colorectal cancers Around 6% are
found as high penetrant disease-causing mutations in genes correlated to hereditary polyposis or
hereditary non-polyposis syndromes. The aim of this thesis was to identify new causative genes and
variants and also mutation mechanisms in families presenting a polyposis, atypical polyposis or nonpolyposis
CRC phenotype.
In classical familial adenomatous polyposis (FAP) 100% of the disease-causing mutations were
found in patients from the Swedish Polyposis Registry. The mutation underlying the lowered
expression of the APC gene in one family was identified by SNP array analysis, the mutation was a
split deletion of 61Kb including half of the promoter 1B. Investigation of the significance of this
promoter for expression of the APC gene demonstrated considerably higher expression compared
with the established promoter 1A.
In order to establish a sensitive method for mosaic-mutation detection a comparison of mutation
detection methods was performed. Low frequency mosaic mutations were detected down to 1 % by
use of massively parallel sequencing (MPS). Whole exome sequencing in four families with
attenuated FAP (AFAP), atypical polyposis or non-polyposis syndromes identified two high
penetrant disease-causing mutations. One was found in the upstream regulatory region of
GREM1and one in the exonuclease domain of POLE. Variants in low-penetrant genes possibly
contributing to CRC development were also proposed from the exome sequencing and gene
specific analyses of 107 patients. Sixty-seven of these patients were analyzed in a panel of 19
selected CRC predisposing genes. Truncating mutations were found in the BMPR1A and SMAD4
genes in patients with a classical FAP, atypical FAP or non-polyposis phenotype. Classification of
found non-synonymous variants was also performed.
In summary, using a combination of different molecular screening techniques, 100% of diseasecausing
mutations in classical FAP can be found. With MPS it is possible to detect low-frequency
mosaic mutations down to 1% by absolute quantification. Whole exome analyses identified
mutations in the new causative genes POLE and GREM1. It was also concluded that patients
without identified mutations, based on phenotypical CRC classification, can have mutations in
genes not included in the primary routine analysis. These results will lead to improved mutation
detection analysis for diagnostic and carrier testing. | sv |
| dc.language.iso | eng | sv |
| dc.relation.haspart | I. Clinical characterization and the mutation spectrum in Swedish adenomatous polyposis families.
Kanter-Smoler G, Fritzell K, Rohlin A, Engwall Y, Hallberg B, Bergman A, Meuller J, Grönberg H, Karlsson P, Björk J, Nordling M.
BMC Med. 2008 Apr 24;6:10. doi: 10.1186/1741-7015-6-10.
::PMID::18433509 | sv |
| dc.relation.haspart | II. Inactivation of promoter 1B of APC causes partial gene silencing: evidence for a significant role of the promoter in regulation and causative of familial adenomatous polyposis.
Rohlin A, Engwall Y, Fritzell K, Göransson K, Bergsten A, Einbeigi Z, Nilbert M, Karlsson P, Björk J, Nordling M.
Oncogene. 2011 Dec 15;30(50):4977-89. doi: 10.1038/onc.2011.201. Epub 2011 Jun 6.
::PMID::21643010 | sv |
| dc.relation.haspart | III. Parallel sequencing used in detection of mosaic mutations: comparison with four diagnostic DNA screening techniques.
Rohlin A, Wernersson J, Engwall Y, Wiklund L, Björk J, Nordling M.
Hum Mutat. 2009 Jun;30(6):1012-20. doi: 10.1002/humu.20980.
::PMID::19347965 | sv |
| dc.relation.haspart | IV. Rohlin A, Eiengård F, Lundstam U, Zagoras T, Nilsson S, Edsjö A, Pedersen J,
Svensson JH, Skullman S, Karlsson GB, Björk J, Nordling M. Whole exome sequencing
in hereditary colorectal cancer syndromes; Identification of causative mutations
and contributing variants. Submitted Manuscript | sv |
| dc.relation.haspart | V. A mutation in POLE predisposing to a multi-tumour phenotype.
Rohlin A, Zagoras T, Nilsson S, Lundstam U, Wahlström J, Hultén L, Martinsson T, Karlsson GB, Nordling M.
Int J Oncol. 2014 Jul;45(1):77-81. doi: 10.3892/ijo.2014.2410. Epub 2014 Apr 29.
PMID: 24788313 | sv |
| dc.relation.haspart | VI. Rohlin A, Rambech E, Kvist A, Eiengård F, Wernersson J, Lundstam U, Zagoras
T, Törngren T, Borg Å, Björk J, Nilbert M, Nordling M. A validated multigene
panel for colorectal cancer syndromes Manuscript | sv |
| dc.subject | Hereditary Colorectal cancer | sv |
| dc.subject | FAP | sv |
| dc.subject | AFAP | sv |
| dc.subject | mutations | sv |
| dc.subject | mosaic mutation | sv |
| dc.subject | exome sequencing | sv |
| dc.subject | massively parallel sequencing | sv |
| dc.subject | next generation sequencing | sv |
| dc.subject | atypical polyposis | sv |
| dc.subject | APC | sv |
| dc.subject | POLE | sv |
| dc.subject | GREM1 | sv |
| dc.subject | PPAP | sv |
| dc.title | Hereditary Colorectal Cancer; Identification, Characterization and Classification of Mutations | sv |
| dc.type | text | eng |
| dc.type.svep | Doctoral thesis | eng |
| dc.gup.mail | anna.rohlin@vgregion.se | sv |
| dc.type.degree | Doctor of Philosophy (Medicine) | sv |
| dc.gup.origin | University of Gothenburg. Sahlgrenska Academy | sv |
| dc.gup.department | Institute of Biomedicine. Department of Medical Genetics | sv |
| dc.gup.defenceplace | Fredagen den 16 januari 2015 kl. 9.00, Hörsal Arvid Carlsson, Academicum, Medicinaregatan 3 | sv |
| dc.gup.defencedate | 2015-01-16 | |
| dc.gup.dissdb-fakultet | SA | |
