Chromosomal fragile site
Chromosomal Fragile Site
A chromosomal fragile site is a specific area on a chromosome that tends to form gaps or breaks when cells are cultured under certain conditions. These sites are considered to be sensitive to replication stress and can be indicative of genomic instability. Fragile sites are classified into two main categories: common fragile sites and rare fragile sites.
Types of Fragile Sites
Common Fragile Sites
Common fragile sites are present in all individuals and are considered a normal part of the human genome. They are often found in regions that are prone to breakage under conditions of replication stress, such as when cells are treated with aphidicolin, a DNA polymerase inhibitor. These sites are thought to play a role in cancer development, as they can lead to chromosomal rearrangements and gene amplification.
Rare Fragile Sites
Rare fragile sites are less common and are often associated with specific genetic disorders. They are usually inherited in a Mendelian fashion and can be induced by specific culture conditions, such as the presence of folate or thymidylate synthase inhibitors. One of the most well-known rare fragile sites is the fragile X site on the X chromosome, which is associated with fragile X syndrome, a genetic condition that causes intellectual disability.
Mechanisms of Fragility
The mechanisms underlying chromosomal fragility are not fully understood, but they are believed to involve problems with DNA replication and repair. Fragile sites often contain sequences that are difficult to replicate, such as AT-rich regions, trinucleotide repeats, or palindromic sequences. These sequences can form secondary structures that stall the replication fork, leading to gaps or breaks in the chromosome.
Clinical Significance
Chromosomal fragile sites are of clinical interest because of their association with genetic disorders and cancer. For example, the fragile X site is linked to fragile X syndrome, the most common inherited cause of intellectual disability. In cancer, common fragile sites are often sites of chromosomal translocations, deletions, and amplifications, which can lead to the activation of oncogenes or the inactivation of tumor suppressor genes.
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