Get in touch

Until now, it had been thought that only already activated ATM could be recruited to the DNA damage sites, but the Salk’s team findings, which are reported in the Oct. 25 advanced online edition of Nature Cell Biology, show just the opposite.

“We found that efficient ATM activation occurs only when it has physical contact with areas flanking the DNA breaks,” says postdoctoral researcher and lead author Zhongsheng You, Ph.D. “When we blocked access to the adjoining regions, ATM activation was severely reduced,” he adds.

“Activating ATM ‘on scene’ ensures a strong local DNA repair response, while the extent of the global response will depend on the number of double strand breaks within the cell,” according to senior author Tony Hunter, Ph.D., a professor in the Molecular and Cell Biology Laboratory.

Our genetic material or DNA is constantly damaged by both external sources such as the sun’s ultraviolet rays, and internal sources such as reactive oxygen species. Fortunately, cells have developed elegant surveillance systems to detect and repair the damaged DNA.

In the event of the most dangerous form of DNA damage, double-strand breaks, ATM coordinates the cellular response. ATM functions as a kinase — an enzyme that can install phosphate molecules on its substrates — and activates a wide variety of DNA repair enzymes and cell-cycle regulators by phosphorylating them. As a result, the cell cycle is halted until DNA repair is completed to prevent cells from passing on damaged genetic material, which could lead to cancer-causing mutations. If the damage is beyond repair, cells undergo programmed cell death.

A lack or deficiency of functional ATM (ataxia-teleangiectasia, mutated) is the underlying cause for a debilitating human genetic disease called ataxia-teleangiectasia. It is characterized by a wide spectrum of defects including neurodegeneration leading to uncoordinated or ataxic movements, immune dysfunction, radiosensitivity and cancer predisposition.

A lot of work has centered on the downstream targets of ATM since its discovery more than a decade ago. But the precise mechanism by which damaged DNA activates ATM had remained unclear. To address this issue You took advantage of a unique property of cellular extracts prepared from unfertilized frog eggs. Adding linear DNA fragments to these extracts mimics DNA double-strand breaks in cellular DNA: ATM rapidly self-activates and slams the brake on the cell cycle machinery.

The Salk scientist happened to have DNA fragments of different lengths (80 bps to 10 kbps) at hand and just added the same number of molecules, assuming that it was the number of ends or “breaks” that mattered and not their size. Not so. “The longer, the better,” says You to describe what he found when he assessed the ability of the DNA fragments in activating ATM. “Efficient ATM activation critically depends on both the number of DNA breaks and the total length of damaged DNA molecules.”

This puzzling observation led him to ask what role the intact DNA neighborhood played in the activation process. His experiments, he says, suggest that ATM is cooperatively activated after being recruited to the regions flanking broken DNA ends. “This mechanism directly couples ATM activation with damaged DNA and ensures that ATM is rapidly activated in response to just a few DNA breaks,” he explains.

Adds Hunter: “Recruiting ATM not only to the break itself but to the flanking regions as well, amplifies the signal from a small number of breaks to generate robust cell cycle block and DNA repair responses.”

DNA is not just floating around inside a cell’s nucleus, instead it is tightly wound around proteins known as histones, which are lined up along the DNA molecule like beads on a string. The whole assembly is collectively known as chromatin. “Our findings suggest that an important signal eliciting the DNA damage response emanates from modified chromatin flanking the DNA breaks in addition to that generated by the primary DNA lesions themselves,” says Hunter.

Source: Salk Institute

Two proteins found on telomeres control DNA damage response pathways
No sooner had cells evolved linear chromosomes than they had a life-threatening problem to solve. To the machinery that repairs broken DNA, chromosome ends look a lot like breaks in need of mending, so they could elicit a DNA damage response that would ultimately be lethal to cells. Telomeres, segments of DNA that sit at the ends of chromosomes, resolve this situation by protecting chromosome ends from being mistaken for DNA breaks.
Chromatin remodeling complex connected to DNA damage control
When molecular disaster strikes, causing structural damage to DNA, players in two important pathways talk to each other to help contain the wreckage, scientists at The University of Texas M. D. Anderson Cancer Center report in the August edition of Cell.
Critical protein prevents DNA damage from persisting through generations
A protein long known to be involved in protecting a cell from genetic damage has been found to play an even more important role in protecting the cell’s offspring. New research shows that the protein, known as ATM, is not only vital for helping repair double-stranded breaks in the DNA of immune cells, but is also part of a system that prevents genetic damage from being passed on when the cells divide.
Scientists discover role of enzyme in DNA repair
Scientists from the National Institute of Arthritis and Musculoskeletal and Skin Diseases (NIAMS), National Cancer Institute (NCI), and Integrative Bioinformatics Inc. have made an important discovery about the role of an enzyme called ataxia telangiectasia mutated protein (ATM) in the body’s ability to repair damaged DNA. NIAMS and NCI are part of the National Institutes of Health (NIH).
Repair of DNA by Brca2 gene prevents medulloblastoma
Investigators at St. Jude Children's Research Hospital have gained some of the first major insights into how certain genes known to prevent cancer also guide the normal development of the nervous system before birth and during infancy by repairing DNA damage.
DNA repair proteins monitored at double-strand break
Investigators at St. Jude Children's Research Hospital had a molecule’s eye view of the human cell’s DNA repair kit as it assembled on a double-strand break to link together the broken ends. Double-strand breaks are ruptures that cut completely across the twisted, ladder-like structure of DNA, breaking it into two pieces.
DNA Repair in Mammal Embryos Is a Matter of Timing
Investigators at St. Jude Children's Research Hospital have discovered that the cells of the developing nervous system of the mammalian embryo have an exquisite sense of timing when it comes to fixing broken chromosomes: the cells use one type of repair mechanism during the first half of development and another during the second half.
Refusal of suicide order: Why tumor cells become resistant
Cells with irreparable DNA damage normally induce programmed cell death, or apoptosis. However, this mechanism often fails in tumor cells so that transformed cells are able to multiply and spread throughout the body. Scientists at the German Cancer Research Center (Deutsches Krebsforschungszentrum, DKFZ) have now discovered a possible cause of this failure. Tumor cells simply degrade a protein that triggers apoptosis in the case of DNA damage. Blocking this protein degradation might set apoptosis back in operation and, thus, increase the effectiveness of radiotherapy or chemotherapy. The researchers have now published their results in Nature Cell Biology.

Get in touch

Related stories:

News discussion: