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Ask a scientist

Ever wish you could grill a scientist about the latest biomedical discoveries and trends? Here's your chance. Email your questions to webmaster@wi.mit.edu and we'll post brief responses from researchers.

In the type of cell division that forms eggs and sperm, replication of DNA is immediately followed by an exchange of genetic material between matching paternal and maternal chromosomes. How do matching chromosomes recognize each other and stick together to ensure that genes are swapped properly?

—Katarzyna Drzewicka, student, Poland

Andreas Hochwagen Response by Andreas Hochwagen
Whitehead Fellow

Your question is a good one. How matching chromosomes find each other before they are distributed during meiosis and packaged into sperm or eggs is still not very well understood. A number of labs around the world, including my own here at the Whitehead, are conducting experiments to investigate this process.

The problem of correctly pairing up matching DNA sequences is profound. Even small genomes contain millions of base pairs of DNA (the baker's yeast genome, which we use for our studies, contains about 12 million). For small organisms, the process of aligning the matching sequences is comparable to finding matching book pages in two piles of about 40,000 pages. For a human cell with a genome of about 3 billion base pairs, this amounts to about 10 million pages in each pile. Yet human cells complete this task in two to three days and budding yeast cells take only about one hour.

There are several mechanisms that appear to collaborate in rapidly sorting the DNA and aligning chromosomes. Some are working at the level of entire chromosomes. For example, in many organisms the chromosome ends get bundled into a conformation known as the "bouquet" prior to meiosis. It is thought that this spatial restriction of chromosomes helps to reduce the space that needs to be searched for a matching partner.

Furthermore, some organisms, such as fruit flies or round worms, appear to have what amounts to identifier sequences. These so-called "pairing centers" are unique for each chromosome. A family of proteins that selectively bind to each of these pairing centers then act as glue to bind matching chromosomes to each other. However, pairing centers have not been found in humans or other mammals.

Large-scale alignment of chromosomes alone is not sufficient to correctly link meiotic chromosomes together because chromosomes also have to be paired at the DNA sequence level. The best understood mechanism involves the formation of single-strandedDNA at spots where the doublestranded structure breaks down. The sequences of these stretches of single-stranded DNA are then used to scan the genome (although how this scanning actually works on a mechanistic level is still not known).

The scanning is highly efficient but also quite error-prone because only short sequence stretches are analyzed by the cell. We know this because the cell occasionally makes mistake, pairing up matching sequences from the wrong chromosomesf there are multiple identical short sequences dispersed throughout the genome. It is thought that the larger-scale pairing mechanisms help to reduce the occurrence of these incorrect pairings by placing the matching chromosomes in each other's vicinity.

In summary, while we have some idea of how the process of chromosome pairing works during meiosis, more experiments will be necessary to get an understanding of how these search mechanisms actually conduct their queries. An important question, because after all, these mechanisms ultimately make sure that sperm and eggs get the correct number of chromosomes.


Last updated July 16, 2007

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