Your search keyword '"fragile sites"' showing total 8 results

1. Breakages at common fragile sites set boundaries of amplified regions in two leukemia cell lines K562 – Molecular characterization of FRA2H and localization of a new CFS FRA2S

Author

Pelliccia, Franca, Bosco, Nazario, and Rocchi, Angela

Subjects

*LEUKEMIA, *CELL lines, *GENE amplification, *HUMAN genome, *CANCER cells, *HUMAN chromosomes, *NUCLEOTIDE sequence

Abstract

Abstract: Genome amplification is often observed in human tumors. The breakage–fusion–bridge (BFB) cycle is the mechanism that often underlies duplicated regions. Some research has indicated common fragile sites (CFS) as possible sites of chromosome breakages at the origin of BFB cycles. Here we searched two human genome regions known as amplification hot spots for any DNA copy number amplifications by analyzing 21 cancer cell lines to investigate the relationship between genomic fragility and amplification. We identified a duplicated region on a chromosomes der(2) present in the karyotype of two analysed leukemia cell lines K562. The two duplicated regions are organized into large palindromes, which suggests that one BFB cycle has occurred. Our findings show that the three breakpoints are localized in the sequence of three CFSs: FRA2H (2q32.1–q32.2), which here has been characterized molecularly; FRA2S (2q22.3–q23.3), a newly localized aphidicolin inducible CFS; and FRA2G (2q24.3–q31). [ABSTRACT FROM AUTHOR]

Published

2010

2. Oncosuppressor proteins of fragile sites are reduced in cervical cancer

Author

Giarnieri, Enrico, Zanesi, Nicola, Bottoni, Arianna, Alderisio, Mauro, Lukic, Ankica, Vecchione, Aldo, Ziparo, Vincenzo, Croce, Carlo Maria, and Mancini, Rita

Subjects

*TUMOR suppressor genes, *CERVICAL cancer diagnosis, *GENE expression, *DIAGNOSTIC immunohistochemistry, *DISEASE progression, *SQUAMOUS cell carcinoma, *TUMOR markers, CANCER cytopathology

Abstract

Abstract: FHIT and WWOX are tumor suppressor genes that span the common fragile sites FRA3B and FRA16D, respectively. To analyze possible synergisms among these genes in cervical cancer progression, we considered 159 cervical intraepithelial neoplasias, and 58 invasive squamous cell carcinomas of the uterine cervix. All cases were previously selected as high risk HPV. FHIT and WWOX proteins were examined by immunohistochemistry and their expression was inversely correlated with precancerous vs. invasive lesions. Statistics among biological markers indicated an association between FHIT and WWOX. Protein expression of these two genes was also absent or reduced in cancer cell lines. Thus, WWOX may be considered as a novel important genetic marker in cervical cancer and the association between the altered expression of FHIT and WWOX may be a critical event in the progression of this neoplasia. [Copyright &y& Elsevier]

Published

2010

3. Hepatitis B virus integration, fragile sites, and hepatocarcinogenesis

Author

Feitelson, Mark A. and Lee, Jungmin

Subjects

*LIVER diseases, *HEPATITIS B, *VIRAL hepatitis, *TUMOR suppressor genes

Abstract

Abstract: Chronic liver disease associated with long term hepatitis B virus (HBV) infection contributes importantly to the development of hepatocellular carcinoma (HCC). A salient feature of these chronic infections is the integration of subgenomic HBV DNA fragments into many different locations within the host DNA, suggesting that integration is random. Although this may promote genetic instability during liver regeneration which accompanies a bout of chronic liver disease, the actual role of integrated HBV DNA in hepatocarcinogenesis is uncertain. Importantly, most integration events retain the HBV open reading frame encoding the HBx antigen (HBxAg), which is the virus contribution to HCC. In addition, many integration events reported in the literature occur near or within fragile sites or other cancer associated regions of the human genome that are prone to instability in tumor development and progression. Genetic instability associated with integration potentially alters the expression of oncogenes, tumor suppressor genes, and microRNAs (miRNAs) that may contribute importantly to tumorigenesis. If so, then selected integration events may alter pathways that are rate limiting in hepatocarcinogenesis, thereby providing targets with diagnostic/prognostic potential and for therapeutic intervention. [Copyright &y& Elsevier]

Published

2007

4. Chromatin structure of human chromosomal fragile sites

Author

Wang, Yuh-Hwa

Subjects

*CHROMATIN, *KARYOKINESIS, *CELL lines, *CHROMOSOMES

Abstract

Abstract: Cytological appearance of fragile sites as non-staining gaps in metaphase chromosomes suggests an abnormality in chromatin structure. Studies of fragile sites at three levels of chromosome organization: (1) examining the ability of DNA derived from fragile sites to form nucleosomes-the basic structural element of chromosomes, (2) probing the arrangement of nucleosome arrays over fragile sites in fragile site-expressing cell lines, and (3) visualizing fragile sites in higher-order chromatin organization, reveal an unusual chromatin structure associated with fragile sites. This fragile site-associated chromatin structure might play an active role in DNA metabolic processes such as replication, transcription, repair and recombination, which are closely linked to the instability of fragile sites. [Copyright &y& Elsevier]

Published

2006

5. Low-frequency common fragile sites: Link to neuropsychiatric disorders?

Author

Savelyeva, Larissa, Sagulenko, Evgeny, Schmitt, Jens Guido, and Schwab, Manfred

Subjects

*GENETIC disorders, *NUCLEOTIDE sequence, *CENTRAL nervous system, *NUCLEIC acids

Abstract

Abstract: Common fragile sites are unstable chromosomal regions that predispose chromosomes to breakage and rearrangements. Recombinogenic DNA sequences encompassing these sites may contribute to both germinal and somatic genomic mutations, and the genomic instability at these regions might cause severe inherited disorders or predispose to cancer. In this review, we discuss the characterization of common fragile site FRA13A within the neurobeachin gene, which is involved in development and function of the central nervous system. We raise the possibility of an implication of common fragile sites in neuropsychiatric disorders and overview previous and recent reports concerning individual variability of expression of common fragile sites in human populations. [Copyright &y& Elsevier]

Published

2006

6. Breakages at common fragile sites set boundaries of amplified regions in two leukemia cell lines K562 - Molecular characterization of FRA2H and localization of a new CFS FRA2S

Author

Angela Rocchi, Franca Pelliccia, and Nazario Bosco

Subjects

Aphidicolin, Cancer Research, Biology, chemistry.chemical_compound, Neoplasms, Gene duplication, Humans, Genetics, cancer cell lines, cancer lines, fragile sites, genome amplification, k562, Chromosomal fragile site, Chromosome Fragile Sites, Breakpoint, Gene Amplification, Chromosome Mapping, Karyotype, Telomere, Oncology, chemistry, Chromosome Fragile Site, Chromosomes, Human, Pair 2, Human genome, Chromosome breakage, K562 Cells

Abstract

Genome amplification is often observed in human tumors. The breakage-fusion-bridge (BFB) cycle is the mechanism that often underlies duplicated regions. Some research has indicated common fragile sites (CFS) as possible sites of chromosome breakages at the origin of BFB cycles. Here we searched two human genome regions known as amplification hot spots for any DNA copy number amplifications by analyzing 21 cancer cell lines to investigate the relationship between genomic fragility and amplification. We identified a duplicated region on a chromosomes der(2) present in the karyotype of two analysed leukemia cell lines K562. The two duplicated regions are organized into large palindromes, which suggests that one BFB cycle has occurred. Our findings show that the three breakpoints are localized in the sequence of three CFSs: FRA2H (2q32.1-q32.2), which here has been characterized molecularly; FRA2S (2q22.3-q23.3), a newly localized aphidicolin inducible CFS; and FRA2G (2q24.3-q31).

Published

2010

7. Oncosuppressor proteins of fragile sites are reduced in cervical cancer

Author

Rita Mancini, Enrico Giarnieri, Nicola Zanesi, Mauro Alderisio, Carlo M. Croce, Arianna Bottoni, Aldo Vecchione, A. Lukic, and Vincenzo Ziparo

Subjects

Oncology, WWOX, Cancer Research, medicine.medical_specialty, Cell, Blotting, Western, Down-Regulation, Uterine Cervical Neoplasms, Biology, Article, FHIT, Internal medicine, Cell Line, Tumor, medicine, Biomarkers, Tumor, Humans, cervical neoplasia, neoplasms, Cervical cancer, tumor suppressors, Chromosomal fragile site, Chromosome Fragile Sites, Tumor Suppressor Proteins, fragile sites, immunohistochemistry, medicine.disease, Immunohistochemistry, Acid Anhydride Hydrolases, Neoplasm Proteins, medicine.anatomical_structure, Genetic marker, Chromosome Fragile Site, Cancer research, Female, HeLa Cells

Abstract

FHIT and WWOX are tumor suppressor genes that span the common fragile sites FRA3B and FRA16D, respectively. To analyze possible synergisms among these genes in cervical cancer progression, we considered 159 cervical intraepithelial neoplasias, and 58 invasive squamous cell carcinomas of the uterine cervix. All cases were previously selected as high risk HPV. FHIT and WWOX proteins were examined by immunohistochemistry and their expression was inversely correlated with precancerous vs. invasive lesions. Statistics among biological markers indicated an association between FHIT and WWOX. Protein expression of these two genes was also absent or reduced in cancer cell lines. Thus, WWOX may be considered as a novel important genetic marker in cervical cancer and the association between the altered expression of FHIT and WWOX may be a critical event in the progression of this neoplasia.

Published

2009

8. The expression of fragile sites in lymphocytes of patients with rectum cancer and their first-degree relatives

Author

Berrin Tunca, Abdullah Zorluoglu, Unal Egeli, Omer Yerci, Tuncay Yilmazlar, Ayhan Kızıl, Uludağ Üniversitesi/Tıp Fakültesi/Tıbbi Biyoloji Anabilim Dalı., Uludağ Üniversitesi/Tıp Fakültesi/Cerrahi Anabilim Dalı., Uludağ Üniversitesi/Tıp Fakültesi/Cerrahi Patoloji Anabilim Dalı., Tunca, Berrin, Egeli, Ünal, Zorluoğlu, Abdullah, Yılmazlar, Tuncay, Yerci, Ömer, Kızıl, Ayhan, and ABI-6078-2020

Subjects

Male, Cancer Research, Renal-cell, Colorectal-cancer, Short arm, chemistry.chemical_compound, Homozygous deletions, Lymphocytes, Breast-cancer, Cells, Cultured, Heterozygosity, Chromosomal fragile site, Chromosome Fragile Sites, Fhit gene, Chromosome Breakage, Middle Aged, medicine.anatomical_structure, Oncology, Rectum cancer, Adenocarcinoma, Female, Aphidicolin, Adult, Tumor-cell lines, Rectum, Chromosomal rearrangement, Biology, Caffeine, medicine, Genetic predisposition, Genetic susceptibility, Humans, Genetic Predisposition to Disease, First-degree relatives, Chromosome-3, Metaphase, Aged, Family Health, Lung cancers, Rectal Neoplasms, Chromosome Fragility, Cancer, medicine.disease, chemistry, Bromodeoxyuridine, Case-Control Studies, Immunology, Cancer research, Fragile sites, DNA Damage

Abstract

Fragile sites are non-staining gaps and breaks in specific points of chromosomes. These sites also include acentric fragments, triradial figures and several rearrangements. Although this issue has been controversial recently, they may be related to structural chromosomal rearrangement in some neoplasms. In this study, the expression of fragile sites induced by aphidicolin (Apc), 5-bromodeoxyuridine (BrJU) and caffeine was investigated on prometaphase chromosomes obtained from the peripheral blood lymphocytes of 36 patients with rectum cancer, 30 first-degree relatives and 30 normal healthy controls. The results of the structural chromosome aberrations determined in patients and their first-degree relatives were significantly higher than those in control subjects (P < 0.001). We determined aphidicolin type common fragile sites (1p36, 1p31, 1p21, 1q21, 1q25, 1q44, 2p24, 2q21, 2q33, 2q37, 3p14, 5q21, 5q33, 13q13, 14q24, 16q23 and 18q21). When the rates of sites such as 1p21, 1q25, 2q33, 3p14, 5q21 and 14q24 in patients and in their first-degree relatives were compared with the control group, the difference was statistically significant. Our results indicated an increased genetic instability in patients with rectum cancer and their first degree relatives. Therefore, the increase of fragile site expression may be an important marker showing genetic predisposition to rectum cancer.

Published

2000