Cancer often starts with the reshuffling of DNA鈥攁kin to scrambling the pages of a dictionary. Exactly how this happens has long been a mystery. But researchers in the 不良研究所 College of Biological Sciences have now arrived at one promising explanation.
The problem seems to happen at a critical moment: when the cell is fixing a broken string of DNA. This repair process, called homologous recombination, can go awry, says Wolf-Dietrich Heyer, a Distinguished Professor and chair in the Department of Microbiology and Molecular Genetics.
鈥It鈥檚 counterintuitive,鈥 he says. 鈥A mechanism for maintaining genome stability can actually cause instability.鈥
Heyer and his students have studied this process for years. Their latest discovery, , could shed light on the origins of cancer and of neurodevelopmental disorders such as autism.
Mismatched DNA
Homologous recombination depends on the fact that human cells contain two complete copies of the genome, divided into 23 pairs of matching chromosomes (and when a cell has duplicated its DNA in preparation for dividing, it briefly has four copies of its genome). When the DNA on one chromosome is broken鈥攁 so-called double-stranded break鈥攖he homologous DNA sequence from a matching chromosome can be used as a template to repair the DNA break.
It鈥檚 a difficult task, because before the cell can repair its DNA, its proteins must first find the matching sequence鈥攖he equivalent of finding 鈥渙ne particular piece of hay in a haystack,鈥 says Heyer.
The problem is that some stretches of DNA have more than one match. This is where the repair process sometimes goes astray鈥攖riggering a genomic catastrophe.
The genomes of humans and all other plants, animals and fungi are full of what some researchers call 鈥渏unk鈥 DNA sequences, which are repeated and scattered thousands of times across the genome. If some of these repeats happen to sit near the broken end of the DNA molecule, then the cell鈥檚 proteins might erroneously match the broken DNA to more than one chromosome.
鈥Instead of using a single homologous chromosome, the cell ends up using multiple regions of the genome to repair the broken DNA,鈥 says Diedre Reitz, the postdoctoral fellow in Heyer鈥檚 lab, who is lead author on the new study.
When multiple matches are made, the cell鈥檚 DNA, which is normally a linear molecule similar to a ladder, ends up in a tangle with branches in multiple places. As the cell鈥檚 proteins unwind that tangle, they clip the DNA in the wrong places, introducing numerous errors.
As a result, the DNA thread that was broken ends up spliced onto a sequence that it wasn鈥檛 previously connected to鈥攃reating an error called a 鈥渢ranslocation.鈥 At this point, the formerly intact DNA strands that were used as repair templates are now broken off鈥攔equiring another round of repair鈥攚ith the potential for compounding errors.
鈥This process can generate a cascade of re-arrangements,鈥 says Heyer, as one botched repair leaves newly broken DNA threads鈥攚hich themselves are repaired incorrectly鈥攑roducing yet more broken threads.
The newly published paper shows that these DNA breaks and incorrect repairs happen in Saccharomyces cerevisiae yeast, an established model in genomics research. Given the evolutionary similarities of the DNA repair proteins between yeast and animals, this may also happen in human disease.
鈥This signature has been observed in many cancers, and in people with certain developmental problems,鈥 says Heyer. 鈥They have what are essentially shattered genomes, in which the DNA of affected cells has dozens or even hundreds of individual breaks and re-arrangements.鈥
This genome shuffling plays a fundamental role in generating cancer cells. So-called tumor suppressor genes, which prevent uncontrolled cell division, can be lost. And 鈥渙ncogenes,鈥 which promote rapid cell division, can be turned on at full blast.
Surprising pathways
This new research builds on an experimental yeast model that was first by Aur猫le Piazza, while he was a post-doctoral fellow in Heyer鈥檚 lab at 不良研究所.
Piazza, who is now a research team leader at the Ecole Normale Sup茅rieure in Lyon, France, also played a pivotal role in the new research. He further adapted his experimental system, using a DNA method called polymerase chain reaction (PCR) to detect DNA repair errors that are vanishingly rare.
The new experiments revealed that these errors in DNA repair can happen through two distinct pathways. One pathway, which was expected, requires the cell to synthesize new DNA, says Piazza. 鈥But you can also get DNA re-arrangements that are massive, but independent of DNA synthesis,鈥 he says鈥攁nd this was a surprise.
It鈥檚 an important discovery because DNA re-arrangements, and cancer, often arise in cells that don鈥檛 normally have the capacity to divide, or synthesize new DNA. The discovery could also be important for understanding autism and other neurodevelopmental diseases: patients with these conditions are sometimes found to harbor DNA re-arrangements in their nerve cells鈥攚hich also tend not to synthesize DNA. In fact, these neural disorders in some of the same genes as cancer.
The newly identified pathways generate specific fingerprints in the DNA sequence. Reitz, Heyer, and their colleagues are starting to look for those fingerprints in tumor samples from cancer patients. Finding them would provide evidence that what they discovered in yeast really could be an important trigger for human disease 鈥 an insight which may one day even affect treatment decisions.
Media Resources
Douglas Fox is a freelance science writer based in the San Francisco Bay Area.
(Genes & Development 2023)
(Cell 2017)
(Trends in Genetics 2016)