Genome complexity: forming chromosomes (Introduction)

by David Turell , Tuesday, March 25, 2025, 18:53 (9 days ago) @ David Turell

Latest findings:

https://www.sciencedaily.com/releases/2025/03/250324113645.htm

"To prepare the 46 chromosomes of a human cell for transport to the daughter cells during cell division, each chromosome forms a compact X-shaped structure with two rod-like copies. How the cell achieves this feat remains largely unknown.

"Now, for the first time, EMBL scientists have directly observed this process in high resolution under the microscope using a new chromatin tracing method. The new study shows that the long DNA molecules of each chromosome form a series of overlapping loops during cell division that repel each other. As a result of this repulsion, the DNA loops then stack up to form rod-shaped chromosomes.

"Scientists have long hypothesised the importance of DNA loops in building and maintaining chromosomal structure. First identified in the 1990s, condensins are large protein complexes that bind DNA during cell division and extrude it to create loops of varying sizes. Previous studies from EMBL have shed light on the structural mechanics of this process and their essential role in packing chromosomes into forms that can be easily moved between cells.

"In fact, mutations in condensin structure can result in severe chromosome segregation defects and lead to cell death, cancer formation, or rare developmental disorders called 'condensinopathies'.

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"...This technique, called LoopTrace, helped the researchers directly observe DNA in dividing cells as it progressively formed loops and folds.

"'Andreas and I were now able to visualise the structure of chromosomes as they started to change shape," said Beckwith. "This was crucial for understanding how the DNA was folded by the condensin complexes."

"From their data, the scientists realised that during cell division, DNA forms loops in two stages. First, it forms stable large loops, which then subdivide into smaller, short-lived nested loops, increasing the compaction at each stage. Two types of condensin protein complexes enable this process.

"...First, as observed, DNA forms overlapping loops -- first large and then small -- across its length with the help of Condensins. Second, these loops repel each other due to their structure and the chemistry of DNA. When the scientists fed these two assumptions into their model, they found that this was sufficient to give rise to a rod-shaped chromosome structure.

"'We realised that these condensin-driven loops are much larger than previously thought, and that it was very important that the large loops overlap to a significant extent," said Beckwith. "Only these features allowed us to recapitulate the native structure of mitotic chromosomes in our model and understand how they can be segregated during cell division."

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"In the meantime, a second study from the Ellenberg Team, led by Andreas Brunner and recently published in the Journal of Cell Biology, shows that the nested loop mechanism is fundamental to the biology of cells, and continues during the cell's growth phase with another family of DNA loop forming protein complexes, called cohesins.

"'We were surprised to find that the same core principle of sequential and hierarchical DNA loop formation is used to either tightly pack chromosomes during division into safely movable entities, or to unpack them afterwards to read out the information they contain," said Ellenberg. "In the end, small, but key mechanistic differences, such as the non-overlapping nature of cohesin-driven loops compared to the strongly overlapping condensin-driven loops might be sufficient to explain the vast differences that we see in the shape the genome takes in interphase and mitosis under the microscope.'"

Comment: this very precise packing process had to be designed. I'm surprised that the role of histones as spools for the DNA is not mentioned.