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Neoplasma Vol.61, No.3, p.283-290, 2014 |
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Title: Intestinal flora of FAP patients containing APC-like sequences | ||
Author: K. Hainova, Z. Adamcikova, S. Ciernikova, V. Stevurkova, S. Tyciakova, V. Zajac | ||
Abstract: Colorectal cancer mortality is one of the most common cause of cancer-related mortality. A multiple risk factors are associated with colorectal cancer, including hereditary, enviromental and inflammatory syndromes affecting the gastrointestinal tract. Familial adenomatous polyposis (FAP) is characterized by the emergence of hundreds to thousands of colorectal adenomatous polyps and FAP syndrome is caused by mutations within the adenomatous polyposis coli (APC) tumor suppressor gene. We analyzed 21 rectal bacterial subclones isolated from FAP patient 41-1 with confirmed 5bp ACAAA deletion within codons 1060-1063 for the presence of APC-like sequences in longest exon 15. The studied section was defined by primers 15Efor-15Erev, what correlates with mutation cluster region (MCR) in which the 75% of all APC germline mutations were detected. More than 90% homology was showed by sequencing and subsequent software comparison. The expression of APC-like sequences was demostrated by Western blot analysis using monoclonal and polyclonal antibodies against APC protein. To study missing link between the DNA analysis (PCR, DNA sequencing) and protein expresion experiments (Western blotting) we analyzed bacterial transcripts containing the 15Efor-15Erev sequence of APC gene by reverse transcription-PCR, what indicated that an APC gene derived fragment may be produced. We observed 97-100 % homology after computer comparison of cDNA PCR products. Our results suggest that presence of APC-like sequences in intestinal/rectal bacteria is enrichment of bacterial genetic information in which horizontal gene transfer between humans and microflora play an important role. |
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Keywords: colorectal cancer, familial adenomatous polyposis, bacterial flora, APC-like sequences, APC-like protein | ||
Published online: 31-Jan-2014 | ||
Year: 2014, Volume: 61, Issue: 3 | Page From: 283, Page To: 290 | |
doi:10.4149/neo_2014_036 |
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