Sequence and structural variation in the genome of the Biomphalaria glabrata embryonic (Bge) cell line
Abstract Background The aquatic pulmonate snail Biomphalaria glabrata is a significant vector and laboratory host for the parasitic flatworm Schistosoma mansoni, an etiological agent for the neglected tropical disease schistosomiasis. Much is known regarding the host-parasite interactions of these t...
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doaj-a28290239d51425b851a562c2bba8d692020-11-25T00:48:18ZengBMCParasites & Vectors1756-33052018-09-0111111210.1186/s13071-018-3059-2Sequence and structural variation in the genome of the Biomphalaria glabrata embryonic (Bge) cell lineNicolas J. Wheeler0Nathalie Dinguirard1Joshua Marquez2Adrian Gonzalez3Mostafa Zamanian4Timothy P. Yoshino5Maria G. Castillo6Department of Pathobiological Sciences, School of Veterinary Medicine, University of WisconsinDepartment of Pathobiological Sciences, School of Veterinary Medicine, University of WisconsinDepartment of Biology, New Mexico State UniversityDepartment of Biology, New Mexico State UniversityDepartment of Pathobiological Sciences, School of Veterinary Medicine, University of WisconsinDepartment of Pathobiological Sciences, School of Veterinary Medicine, University of WisconsinDepartment of Biology, New Mexico State UniversityAbstract Background The aquatic pulmonate snail Biomphalaria glabrata is a significant vector and laboratory host for the parasitic flatworm Schistosoma mansoni, an etiological agent for the neglected tropical disease schistosomiasis. Much is known regarding the host-parasite interactions of these two organisms, and the B. glabrata embryonic (Bge) cell line has been an invaluable resource in these studies. The B. glabrata BB02 genome sequence was recently released, but nothing is known of the sequence variation between this reference and the Bge cell genome, which has likely accumulated substantial genetic variation in the ~50 years since its isolation. Results Here, we report the genome sequence of our laboratory subculture of the Bge cell line (designated Bge3), which we mapped to the B. glabrata BB02 reference genome. Single nucleotide variants (SNVs) were predicted and focus was given to those SNVs that are most likely to affect the structure or expression of protein-coding genes. Furthermore, we have highlighted and validated high-impact SNVs in genes that have often been studied using Bge cells as an in vitro model, and other genes that may have contributed to the immortalization of this cell line. We also resolved representative karyotypes for the Bge3 subculture, which revealed a mixed population exhibiting substantial aneuploidy, in line with previous reports from other Bge subcultures. Conclusions The Bge3 genome differs from the B. glabrata BB02 reference genome in both sequence and structure, and these are likely to have significant biological effects. The availability of the Bge3 genome sequence, and an awareness of genomic differences with B. glabrata, will inform the design of experiments to understand gene function in this unique in vitro snail cell model. Additionally, this resource will aid in the development of new technologies and molecular approaches that promise to reveal more about this schistosomiasis-transmitting snail vector.http://link.springer.com/article/10.1186/s13071-018-3059-2BgeGenome sequenceVariant callingKaryotypeBiomphalaria glabrataSchistosoma mansoni |
collection |
DOAJ |
language |
English |
format |
Article |
sources |
DOAJ |
author |
Nicolas J. Wheeler Nathalie Dinguirard Joshua Marquez Adrian Gonzalez Mostafa Zamanian Timothy P. Yoshino Maria G. Castillo |
spellingShingle |
Nicolas J. Wheeler Nathalie Dinguirard Joshua Marquez Adrian Gonzalez Mostafa Zamanian Timothy P. Yoshino Maria G. Castillo Sequence and structural variation in the genome of the Biomphalaria glabrata embryonic (Bge) cell line Parasites & Vectors Bge Genome sequence Variant calling Karyotype Biomphalaria glabrata Schistosoma mansoni |
author_facet |
Nicolas J. Wheeler Nathalie Dinguirard Joshua Marquez Adrian Gonzalez Mostafa Zamanian Timothy P. Yoshino Maria G. Castillo |
author_sort |
Nicolas J. Wheeler |
title |
Sequence and structural variation in the genome of the Biomphalaria glabrata embryonic (Bge) cell line |
title_short |
Sequence and structural variation in the genome of the Biomphalaria glabrata embryonic (Bge) cell line |
title_full |
Sequence and structural variation in the genome of the Biomphalaria glabrata embryonic (Bge) cell line |
title_fullStr |
Sequence and structural variation in the genome of the Biomphalaria glabrata embryonic (Bge) cell line |
title_full_unstemmed |
Sequence and structural variation in the genome of the Biomphalaria glabrata embryonic (Bge) cell line |
title_sort |
sequence and structural variation in the genome of the biomphalaria glabrata embryonic (bge) cell line |
publisher |
BMC |
series |
Parasites & Vectors |
issn |
1756-3305 |
publishDate |
2018-09-01 |
description |
Abstract Background The aquatic pulmonate snail Biomphalaria glabrata is a significant vector and laboratory host for the parasitic flatworm Schistosoma mansoni, an etiological agent for the neglected tropical disease schistosomiasis. Much is known regarding the host-parasite interactions of these two organisms, and the B. glabrata embryonic (Bge) cell line has been an invaluable resource in these studies. The B. glabrata BB02 genome sequence was recently released, but nothing is known of the sequence variation between this reference and the Bge cell genome, which has likely accumulated substantial genetic variation in the ~50 years since its isolation. Results Here, we report the genome sequence of our laboratory subculture of the Bge cell line (designated Bge3), which we mapped to the B. glabrata BB02 reference genome. Single nucleotide variants (SNVs) were predicted and focus was given to those SNVs that are most likely to affect the structure or expression of protein-coding genes. Furthermore, we have highlighted and validated high-impact SNVs in genes that have often been studied using Bge cells as an in vitro model, and other genes that may have contributed to the immortalization of this cell line. We also resolved representative karyotypes for the Bge3 subculture, which revealed a mixed population exhibiting substantial aneuploidy, in line with previous reports from other Bge subcultures. Conclusions The Bge3 genome differs from the B. glabrata BB02 reference genome in both sequence and structure, and these are likely to have significant biological effects. The availability of the Bge3 genome sequence, and an awareness of genomic differences with B. glabrata, will inform the design of experiments to understand gene function in this unique in vitro snail cell model. Additionally, this resource will aid in the development of new technologies and molecular approaches that promise to reveal more about this schistosomiasis-transmitting snail vector. |
topic |
Bge Genome sequence Variant calling Karyotype Biomphalaria glabrata Schistosoma mansoni |
url |
http://link.springer.com/article/10.1186/s13071-018-3059-2 |
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