Entry - *609190 - ANTI-SILENCING FUNCTION 1B HISTONE CHAPERONE; ASF1B - OMIM

 
 
* 609190

ANTI-SILENCING FUNCTION 1B HISTONE CHAPERONE; ASF1B


Alternative titles; symbols

ANTI-SILENCING FUNCTION 1, S. CEREVISIAE, HOMOLOG OF, B


HGNC Approved Gene Symbol: ASF1B

Cytogenetic location: 19p13.12     Genomic coordinates (GRCh38): 19:14,119,512-14,136,589 (from NCBI)


TEXT

Cloning and Expression

Using TLK1 (608438) and TLK2 (608439) as bait in a yeast 2-hybrid screen of a peripheral lymphocyte cDNA library, Sillje and Nigg (2001) cloned ASF1B and ASF1A (609189). The deduced 203-amino acid ASF1B protein has a calculated molecular mass of 22.4 kD. ASF1B and ASF1A share 71% amino acid identity, and they share about 50% identity with yeast Asf1, which has a C-terminal acidic stretch not found in the human ASF1 proteins.


Gene Function

Sillje and Nigg (2001) found that in vitro translated ASF1A and ASF1B were phosphorylated by TLK1 and TLK2. The levels of ASF1A and ASF1B were unchanged during the cell cycle in synchronized HeLa cells.

Mello et al. (2002) found that ASF1A and ASF1B interacted directly and functioned synergistically with human CAF1 (see 601245) to assemble nucleosomes during nucleotide excision repair in vitro.

Groth et al. (2007) characterized the complex in which the human histone chaperone ASF1 and MCM2-7 (see 116945), the putative replicative helicase, are connected through a histone H3-H4 bridge. Depletion of ASF1 by RNA interference impeded DNA unwinding at replication sites, and similar defects arose from overproduction of new histone H3-H4 that compromised ASF1 function. Groth et al. (2007) concluded that their data link ASF1 chaperone function, histone supply, and replicative unwinding of DNA in chromatin. Groth et al. (2007) proposed that ASF1, as a histone acceptor and donor, handles parental and new histones at the replication fork via an ASF1-(H3-H4)-MCM2-7 intermediate and thus provides a means to fine-tune replication fork progression and histone supply and demand.


Mapping

Hartz (2005) mapped the ASF1B gene to chromosome 19p13.13 based on an alignment of the ASF1B sequence (GenBank AB104486) with the genomic sequence.

REFERENCES

  1. Groth, A., Corpet, A., Cook, A. J. L., Roche, D., Bartek, J., Lukas, J., Almouzni, G. Regulation of replication fork progression through histone supply and demand. Science 318: 1928-1931, 2007. [PubMed: 18096807, related citations] [Full Text]

  2. Hartz, P. A. Personal Communication. Baltimore, Md. 2/3/2005.

  3. Mello, J. A., Sillje, H. H. W., Roche, D. M. J., Kirschner, D. B., Nigg, E. A., Almouzni, G. Human Asf1 and CAF-1 interact and synergize in a repair-coupled nucleosome assembly pathway. EMBO Rep. 3: 329-334, 2002. [PubMed: 11897662, images, related citations] [Full Text]

  4. Sillje, H. H. W., Nigg, E. A. Identification of human Asf1 chromatin assembly factors as substrates of Tousled-like kinases. Curr. Biol. 11: 1068-1073, 2001. [PubMed: 11470414, related citations] [Full Text]


Contributors:
Ada Hamosh - updated : 2/11/2008
Creation Date:
Patricia A. Hartz : 2/3/2005
Edit History:
carol : 03/24/2020
alopez : 02/14/2008
terry : 2/11/2008
mgross : 2/3/2005

* 609190

ANTI-SILENCING FUNCTION 1B HISTONE CHAPERONE; ASF1B


Alternative titles; symbols

ANTI-SILENCING FUNCTION 1, S. CEREVISIAE, HOMOLOG OF, B


HGNC Approved Gene Symbol: ASF1B

Cytogenetic location: 19p13.12     Genomic coordinates (GRCh38): 19:14,119,512-14,136,589 (from NCBI)


TEXT

Cloning and Expression

Using TLK1 (608438) and TLK2 (608439) as bait in a yeast 2-hybrid screen of a peripheral lymphocyte cDNA library, Sillje and Nigg (2001) cloned ASF1B and ASF1A (609189). The deduced 203-amino acid ASF1B protein has a calculated molecular mass of 22.4 kD. ASF1B and ASF1A share 71% amino acid identity, and they share about 50% identity with yeast Asf1, which has a C-terminal acidic stretch not found in the human ASF1 proteins.


Gene Function

Sillje and Nigg (2001) found that in vitro translated ASF1A and ASF1B were phosphorylated by TLK1 and TLK2. The levels of ASF1A and ASF1B were unchanged during the cell cycle in synchronized HeLa cells.

Mello et al. (2002) found that ASF1A and ASF1B interacted directly and functioned synergistically with human CAF1 (see 601245) to assemble nucleosomes during nucleotide excision repair in vitro.

Groth et al. (2007) characterized the complex in which the human histone chaperone ASF1 and MCM2-7 (see 116945), the putative replicative helicase, are connected through a histone H3-H4 bridge. Depletion of ASF1 by RNA interference impeded DNA unwinding at replication sites, and similar defects arose from overproduction of new histone H3-H4 that compromised ASF1 function. Groth et al. (2007) concluded that their data link ASF1 chaperone function, histone supply, and replicative unwinding of DNA in chromatin. Groth et al. (2007) proposed that ASF1, as a histone acceptor and donor, handles parental and new histones at the replication fork via an ASF1-(H3-H4)-MCM2-7 intermediate and thus provides a means to fine-tune replication fork progression and histone supply and demand.


Mapping

Hartz (2005) mapped the ASF1B gene to chromosome 19p13.13 based on an alignment of the ASF1B sequence (GenBank AB104486) with the genomic sequence.

REFERENCES

  1. Groth, A., Corpet, A., Cook, A. J. L., Roche, D., Bartek, J., Lukas, J., Almouzni, G. Regulation of replication fork progression through histone supply and demand. Science 318: 1928-1931, 2007. [PubMed: 18096807] [Full Text: https://doi.org/10.1126/science.1148992]

  2. Hartz, P. A. Personal Communication. Baltimore, Md. 2/3/2005.

  3. Mello, J. A., Sillje, H. H. W., Roche, D. M. J., Kirschner, D. B., Nigg, E. A., Almouzni, G. Human Asf1 and CAF-1 interact and synergize in a repair-coupled nucleosome assembly pathway. EMBO Rep. 3: 329-334, 2002. [PubMed: 11897662] [Full Text: https://doi.org/10.1093/embo-reports/kvf068]

  4. Sillje, H. H. W., Nigg, E. A. Identification of human Asf1 chromatin assembly factors as substrates of Tousled-like kinases. Curr. Biol. 11: 1068-1073, 2001. [PubMed: 11470414] [Full Text: https://doi.org/10.1016/s0960-9822(01)00298-6]


Contributors:
Ada Hamosh - updated : 2/11/2008

Creation Date:
Patricia A. Hartz : 2/3/2005

Edit History:
carol : 03/24/2020
alopez : 02/14/2008
terry : 2/11/2008
mgross : 2/3/2005



NOTE: OMIM is intended for use primarily by physicians and other professionals concerned with genetic disorders, by genetics researchers, and by advanced students in science and medicine. While the OMIM database is open to the public, users seeking information about a personal medical or genetic condition are urged to consult with a qualified physician for diagnosis and for answers to personal questions.
OMIM® and Online Mendelian Inheritance in Man® are registered trademarks of the Johns Hopkins University.
Copyright® 1966-2024 Johns Hopkins University.

NOTE: OMIM is intended for use primarily by physicians and other professionals concerned with genetic disorders, by genetics researchers, and by advanced students in science and medicine. While the OMIM database is open to the public, users seeking information about a personal medical or genetic condition are urged to consult with a qualified physician for diagnosis and for answers to personal questions.
OMIM® and Online Mendelian Inheritance in Man® are registered trademarks of the Johns Hopkins University.
Copyright® 1966-2024 Johns Hopkins University.
Printed: May 17, 2024