Constitutive heterochromatin

C-banding of a human female karyotype showing constitutive heterochromatin[1]

Constitutive heterochromatin domains are regions of DNA found throughout the chromosomes of eukaryotes.[2] The majority of constitutive heterochromatin is found at the pericentromeric regions of chromosomes, but is also found at the telomeres and throughout the chromosomes.[2] In humans there is significantly more constitutive heterochromatin found on chromosomes 1, 9, 16, 19 and on the Y chromosome.[3] Constitutive heterochromatin is composed mainly of high copy number tandem repeats known as satellite repeats, minisatellite and microsatellite repeats, and transposon repeats. In humans these regions account for about 200Mb or 6.5% of the total human genome, but their repeat composition has made it difficult to sequence so only small regions have been sequenced. The Y chromosome is an exception in that it has been sequenced because its repeats do not cause difficulties in finding overlapping regions that are needed for sequencing.[3]

Visualization of constitutive heterochromatin is possible by using the C-banding technique. The regions that stain darker are regions of constitutive heterochromatin.[4] The constitutive heterochromatin stains darker because of the highly condensed nature of the DNA.

Constitutive heterochromatin is not to be confused with faculatitive heterochromatin which is less condensed, less stable, does not stain when using the C-banding technique, and is much less polymorphic.

Possible models for expression of genes found in constitutive heterochromatin.[5]

Function

Constitutive heterochromatin is found more commonly in the periphery of the nucleus attached to the nuclear membrane. This concentrates the euchromatic DNA in the center of the nucleus where it can be actively transcribed. During mitosis it is believed that constitutive heterochromatin is necessary for proper segregation of sister chromatids and centromere function.[6] The repeat sequences found at the pericentromeres is not conserved throughout many species and depends more on the epigenetic modifications for regulation while telomeres show more conserved sequences.[2]

Constitutive heterochromatin was thought to be relatively devoid of genes, but researchers have found more than 450 genes in the heterochromatic DNA of Drosophila melanogaster. [5] These regions are highly condensed and epigenetically modified to prevent transcription. In order for the genes to be transcribed they must have a mechanism to overcome the silencing that occurs in the rest of the heterochromatin. There are many proposed models for how the genes in these regions are expressed, including the insulation, denial, integration, exploitation, and TE restraining models.

In most cases when genes are placed near a region of constitutive heterochromatin their transcription is silenced, this effect is known as position-effect variegation and can lead to a mosaic phenotype.

Replication and Epigenetics

Constitutive heterochromatin is replicated late in S phase of the cell cycle and does not participate in meiotic recombination.

Histone modifications are one of the main ways that the cell condenses constitutive heterochromatin.[7] Three modifications found most commonly in constitutive heterochromatin are:

These modifications are found in other types of DNA as well, but are much more concentrated in regions of constitutive heterochromatin. Cytosine methylation is the most common type of DNA modification although it is not found in all eukaryotes. In humans there is increased methylation at the centromeres and telomeres which are composed of constitutive heterochromatin. These modifications can also be passed through meiotic divisions, mitotic divisions, and then passed on to the offspring.

SUV39H1 is a vital DNA methyltransferase that methylates H3K9, providing a binding spot for Heterochromatin protein 1 (HP1). HP1 is involved in the chromatin condensing process that makes DNA inaccessible for transcription.[8][9]

Diseases of constitutive heterochromatin

Genetic disorders that result from mutations involving the constitutive heterochromatin tend to affect cell differentiation and are inherited in an autosomal recessive manner.[6] Disorders include:

Some cancers show anomalies in the constitutive heterochromatin and the proteins involved in its formation and maintenance.

References

  1. "C-Banding". web.udl.es. Retrieved 2015-12-02.
  2. 1 2 3 Saksouk, Nehmé; Simboeck, Elisabeth; Déjardin, Jérôme (2015-01-15). "Constitutive heterochromatin formation and transcription in mammals". Epigenetics & Chromatin 8. doi:10.1186/1756-8935-8-3. ISSN 1756-8935. PMC 4363358. PMID 25788984.
  3. 1 2 T. Strachan and A. Read (2004). Human Molecular Genetics 3. Garland Publishing. pp. 256–295. ISBN 0-81534182-2.
  4. Angell, Roslyn R.; Jacobs, Patricia A. (1975-12-01). "Lateral asymmetry in human constitutive heterochromatin". Chromosoma 51 (4): 301–310. doi:10.1007/BF00326317. ISSN 0009-5915.
  5. 1 2 Yasuhara, Jiro C.; Wakimoto, Barbara T. (2006-06-01). "Oxymoron no more: the expanding world of heterochromatic genes". Trends in Genetics 22 (6): 330–338. doi:10.1016/j.tig.2006.04.008.
  6. 1 2 Marie-Geneviève Mattei and Judith Luciani. "Heterochromatin, from Chromosome to Protein". Atlas of Genetics and Cytogenetics in Oncology and Haematology. Retrieved 9 November 2015.
  7. Richards, Eric J.; Elgin, Sarah C. R. "Epigenetic Codes for Heterochromatin Formation and Silencing". Cell 108 (4): 489–500. doi:10.1016/S0092-8674(02)00644-X. ISSN 0092-8674. PMID 11909520.
  8. Bártová, Eva; Krejčí, Jana; Harničarová, Andrea; Galiová, Gabriela; Kozubek, Stanislav (2008-08-01). "Histone Modifications and Nuclear Architecture: A Review". Journal of Histochemistry & Cytochemistry 56 (8): 711–721. doi:10.1369/jhc.2008.951251. ISSN 0022-1554. PMC 2443610. PMID 18474937.
  9. Lomberk, Gwen; Wallrath, Lori; Urrutia, Raul (2006-01-01). "The Heterochromatin Protein 1 family". Genome Biology 7 (7): 228. doi:10.1186/gb-2006-7-7-228. ISSN 1465-6906. PMC 1779566. PMID 17224041.
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