Chaenocephalus aceratus Genome sequencing

The Antarctic icefish (Chaenocephalus aceratus) provides several evolutionary models of human disease, including osteopenia, lipid storage diseases, and anemia. For osteopenia, a reduction in bone mineral density, identifying genetic factors in icefish that underlie the loss of bone mineral density...

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Bibliographic Details
Main Author: BGI
Format: Dataset
Language:English
Published: CNGB 2012
Subjects:
Genome sequencing
Monoisolate
Antarctic
The Antarctic
Antarc*
Icefish
Online Access:https://dx.doi.org/10.26036/cnphis0001066
https://db.cngb.org/search/project/PRJNA89117/
id ftdatacite:10.26036/cnphis0001066
record_format openpolar
spelling ftdatacite:10.26036/cnphis0001066 2023-05-15T13:35:42+02:00 Chaenocephalus aceratus Genome sequencing BGI 2012 https://dx.doi.org/10.26036/cnphis0001066 https://db.cngb.org/search/project/PRJNA89117/ en eng CNGB Genome sequencing Monoisolate Dataset dataset ftp://ftp.cngb.org/pub/sra/sra-instant/reads/ByStudy/sra/SRP/SRP015/SRP015692 2012 ftdatacite https://doi.org/10.26036/cnphis0001066 2021-11-05T12:55:41Z The Antarctic icefish (Chaenocephalus aceratus) provides several evolutionary models of human disease, including osteopenia, lipid storage diseases, and anemia. For osteopenia, a reduction in bone mineral density, identifying genetic factors in icefish that underlie the loss of bone mineral density in icefish over evolutionary time can lead to a better understanding of the mechanisms that lead to bone loss over developmental time in aging humans.Antarctic icefish have greatly reduced skeletal mineralization. Skeletal reduction in icefish occurs by at least two mechanisms. The first is by delaying activation of bone mineralization genes, such as co/7a7. This results in a skeleton that is largely cartilaginous. Regulatory genes that control the timing of bone mineralization in icefish are as yet unknown. The second mechanism of icefish skeletal reduction is a decrease in the extent of mineralization in the skeletal elements that do ossify. Little is yet known about factors that control this process. Molecular genetic comparison of icefish to closely related robustly skeletonized fish, such as the rockcod {Notothenia coriiceps), will help identify regulatory factors essential for the maintenance of bone mineral density. Antarctic icefish accumulate lipids in muscle, skeleton, and connective tissue. This phenotype resembles human disease states such as Chanarin-Dorfman syndrome and neutral lipid storage disease with myopathy. Icefish muscle cells are riddled with lipid vesicles but few studies have investigated the molecular genetic mechanisms that cause icefish to accumulate lipid deposits. In humans, such deposits are debilitating, but in icefish, they are favored by natural selection because they make the body less dense, thus facilitating prey capture off the ocean floor. Icefish have lost the ability to form red blood cells resulting in profound anemia. The cost of this disaptation is low due to the high capacity of cold water to dissolve oxygen and adaptive compensatory responses, including changes in the circulatory system that involve low blood viscosity, large bore capillaries, increased vascularity, cardiomegaly, and high blood flow with low pressure. In addition, icefish hemoglobin genes have become pseudo genes. This situation thus provides an opportunity to identify hematopoietic regulatory factors present in rockcod, the "wild-type control" but absent from icefish, the "evolutionary mutant". Such genes become candidates for genes involved in human anemias. A group in Korea is sequencing Notothenia coriiceps, a fish closely related to icefish that possesses a heavily mineralized skeleton, does not accumulate lipids in muscle and bone, and has a high hematocrit. Thus, a comparator genome sequence with the "healthy" phenotype will be available, making the sequencing of the icefish (C. aceratus), our disease model, even more valuable. Dataset Antarc* Antarctic Icefish DataCite Metadata Store (German National Library of Science and Technology) Antarctic The Antarctic
institution Open Polar
collection DataCite Metadata Store (German National Library of Science and Technology)
op_collection_id ftdatacite
language English
topic Genome sequencing
Monoisolate
spellingShingle Genome sequencing
Monoisolate
BGI
Chaenocephalus aceratus Genome sequencing
topic_facet Genome sequencing
Monoisolate
description The Antarctic icefish (Chaenocephalus aceratus) provides several evolutionary models of human disease, including osteopenia, lipid storage diseases, and anemia. For osteopenia, a reduction in bone mineral density, identifying genetic factors in icefish that underlie the loss of bone mineral density in icefish over evolutionary time can lead to a better understanding of the mechanisms that lead to bone loss over developmental time in aging humans.Antarctic icefish have greatly reduced skeletal mineralization. Skeletal reduction in icefish occurs by at least two mechanisms. The first is by delaying activation of bone mineralization genes, such as co/7a7. This results in a skeleton that is largely cartilaginous. Regulatory genes that control the timing of bone mineralization in icefish are as yet unknown. The second mechanism of icefish skeletal reduction is a decrease in the extent of mineralization in the skeletal elements that do ossify. Little is yet known about factors that control this process. Molecular genetic comparison of icefish to closely related robustly skeletonized fish, such as the rockcod {Notothenia coriiceps), will help identify regulatory factors essential for the maintenance of bone mineral density. Antarctic icefish accumulate lipids in muscle, skeleton, and connective tissue. This phenotype resembles human disease states such as Chanarin-Dorfman syndrome and neutral lipid storage disease with myopathy. Icefish muscle cells are riddled with lipid vesicles but few studies have investigated the molecular genetic mechanisms that cause icefish to accumulate lipid deposits. In humans, such deposits are debilitating, but in icefish, they are favored by natural selection because they make the body less dense, thus facilitating prey capture off the ocean floor. Icefish have lost the ability to form red blood cells resulting in profound anemia. The cost of this disaptation is low due to the high capacity of cold water to dissolve oxygen and adaptive compensatory responses, including changes in the circulatory system that involve low blood viscosity, large bore capillaries, increased vascularity, cardiomegaly, and high blood flow with low pressure. In addition, icefish hemoglobin genes have become pseudo genes. This situation thus provides an opportunity to identify hematopoietic regulatory factors present in rockcod, the "wild-type control" but absent from icefish, the "evolutionary mutant". Such genes become candidates for genes involved in human anemias. A group in Korea is sequencing Notothenia coriiceps, a fish closely related to icefish that possesses a heavily mineralized skeleton, does not accumulate lipids in muscle and bone, and has a high hematocrit. Thus, a comparator genome sequence with the "healthy" phenotype will be available, making the sequencing of the icefish (C. aceratus), our disease model, even more valuable.
format Dataset
author BGI
author_facet BGI
author_sort BGI
title Chaenocephalus aceratus Genome sequencing
title_short Chaenocephalus aceratus Genome sequencing
title_full Chaenocephalus aceratus Genome sequencing
title_fullStr Chaenocephalus aceratus Genome sequencing
title_full_unstemmed Chaenocephalus aceratus Genome sequencing
title_sort chaenocephalus aceratus genome sequencing
publisher CNGB
publishDate 2012
url https://dx.doi.org/10.26036/cnphis0001066
https://db.cngb.org/search/project/PRJNA89117/
geographic Antarctic
The Antarctic
geographic_facet Antarctic
The Antarctic
genre Antarc*
Antarctic
Icefish
genre_facet Antarc*
Antarctic
Icefish
op_doi https://doi.org/10.26036/cnphis0001066
_version_ 1766069076937932800

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