Researchers led by San Diego Ludwig Ball Don Cleveland and Peter Campbell of the Sanger Center have uncovered the mystery of how free floating round DNA fragments are found almost exclusively in the cancer cells, directing gene proliferation to generate drug resistance.
The research, published in the journal Nature, provides new insights into how cancers evolve to adapt to changing environments and suggests ways to reduce drug resistance by combining. remedies.
“The fight against drugs is the hardest part of cancer treatment. If it weren’t for drug resistance, many cancer patients would be alive, ”said Ofer Shoshani, a postdoctoral researcher at the Cleveland laboratory and the first author in the study.
Extrachromosomal DNA (ecDNA) are specific circular units of DNA that are not attached to chromosomes, which pack genomic DNA into the nucleus of the cell. ecDNA can contain many copies of cancer genes that help tumors grow and survive.
Understanding the biology and origins of ecDNA took a turn for the worse after a team led by San Diego Ludwig Member Paul Mischel and his colleague Vineet Bafna at the University of California San Diego School of Medicine first reported in 2017 that found in nearly half of all tumor types and plays a major role in the growth and diversity of cancer cells.
In the new study, Shoshani, Cleveland, Campbell and colleagues show that chromothripsis, chromosome breakdown and their recombination in a mobile order, initiate ecDNA formation.
Chromothripsis was first reported in 2011 by a team led by Campbell. Scientists were speculating at the time that chromosomal breakdown could produce circulating DNA fragments to form ecDNA, but this has not been proven to date.
“What we could show is the link between chromosomal disruption and ecDNA formation,” Cleveland said. The team also showed that ecDNA itself can undergo continuous cycles of chromothripsis to spawn reorganized ecDNAs that provide even higher drug protection.
“We’ve seen these pieces grow over time as they break and regenerate. That means that if an ecDNA fragment encodes a gene that encodes for a product that is directly anticancer drug-free, it can make it more and more of it, leading to drug resistance, ”Cleveland said.
“We have now established this in three different methotrexate-resistant cell lines and in biopsies from human colorectal cancer patients that are resistant to BRAF therapy,” Cleveland said.
While chromothripsis occurs naturally in cancer cells, the researchers found that it can also be stimulated by chemotherapeutic drugs such as methotrexate, which kill cell division by damaging the They have DNA.
In addition, the specific type of DNA damage caused by these drugs – breaking both layers of the DNA double helix – allows ecDNA to re-enter into chromosomes.
“We show that when we break a chromosome, these ecDNAs tend to jump into the fracture and seal, serving almost as a‘ DNA call, ’” Shoshani said.
Thus, some of the real drugs used to treat cancer could lead to drug resistance by generating two-stranded DNA fragmentation.
The researchers found that such formation of ecDNA can be prevented by fixing chemotherapeutic drugs with molecules that prevent the DNA fragments generated by chromosomal breakdown from closing into shape circles.
Shoshani showed that, when applied in combination with cancer cells, this strategy inhibited the formation of ecDNA and reduced drug resistance.
“This means that an approach in which we combine DNA repair inhibitors with drugs such as methotrexate or vemurafenib could prevent drug resistance in cancer patients and improve clinical outcomes,” Shoshani said.
“I think the field has accepted that blending medicine is how we are going to generate better outcomes for cancer patients, but this is a unique example of the types of combinations that should be tested,” said Cleveland.
(This story was published from a wire group without text changes. Only the headline was changed.)
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