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DDC
| 660.6 | |
Tác giả CN
| Nguyen, Hoang Danh | |
Nhan đề
| Cloning human Benchwarmer gene (BNCH) harboring E164K in vector pcDNA3.1 by site-directed mutagenesis method / Nguyen Hoang Danh, Vu Minh Thiet | |
Thông tin xuất bản
| Ho Chi Minh city : Nguyen Tat Thanh University, 2020 | |
Mô tả vật lý
| 6 p. | |
Tóm tắt
| Benchwarmer (BNCH) gene encodes an orphan transmembrane transporter belonging to the Major Facilitator Superfamily (MFS), facilitating the transport of ions, amino acids, simple sugars and recently lysolipids. The loss of BNCH function caused lethality in several animal models with neurodegeneration and senescence. At the cellular level, dysregulation of BNCH leads to adverse phenotypes of lysosome and also autophagy (i.e. dyshomeostasis, accumulation of carbohydrates and sphingolipids, and enlarged lysosome). However, the molecular function and ligand of BNCH protein remain to be unrevealed. This study aims to create a radical substitution change in human BNCH coding gene to knock out the protein functions. More specifically, lysine (K) was used to replace the glutamic acid residue 164 (E164K) which is conserved in many animals (fly, zebrafish, mouse and human) and this E164K mutation recapitulated BNCH mutant phenotype. In conclusion, BNCH harboring E164K (BNCH*) was successfully produced by site-directed mutagenesis and cloned into pcDNA.3.1 vector. The construct was transformed into E. coli OmniMAX and that provides a valuable cell assay to search for the molecular ligand of BNCH. | |
Từ khóa tự do
| Cloning | |
Từ khóa tự do
| Benchwarmer | |
Từ khóa tự do
| Đột Biến | |
Từ khóa tự do
| Lysosomal membrane protein | |
Từ khóa tự do
| Plasmid pcDNA3.1 | |
Nguồn trích
| Tạp chí Khoa học và Công nghệ - Đại học Nguyễn Tất Thành 2020tr. 06-11
Số: 12 |
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000
| 00000nab#a2200000ui#4500 |
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| 001 | 28772 |
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| 002 | 9 |
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| 004 | 733D8A7C-BBFA-43C5-A06A-232FCFE3BDF9 |
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| 005 | 202106072218 |
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| 008 | 081223s2020 vm| vie |
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| 009 | 1 0 |
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| 039 | |y20210607221801|zngantk |
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| 082 | |a660.6 |
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| 100 | |aNguyen, Hoang Danh |
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| 245 | |aCloning human Benchwarmer gene (BNCH) harboring E164K in vector pcDNA3.1 by site-directed mutagenesis method / |cNguyen Hoang Danh, Vu Minh Thiet |
|---|
| 260 | |aHo Chi Minh city : |bNguyen Tat Thanh University, |c2020 |
|---|
| 300 | |a6 p. |
|---|
| 520 | |aBenchwarmer (BNCH) gene encodes an orphan transmembrane transporter belonging to the Major Facilitator Superfamily (MFS), facilitating the transport of ions, amino acids, simple sugars and recently lysolipids. The loss of BNCH function caused lethality in several animal models with neurodegeneration and senescence. At the cellular level, dysregulation of BNCH leads to adverse phenotypes of lysosome and also autophagy (i.e. dyshomeostasis, accumulation of carbohydrates and sphingolipids, and enlarged lysosome). However, the molecular function and ligand of BNCH protein remain to be unrevealed. This study aims to create a radical substitution change in human BNCH coding gene to knock out the protein functions. More specifically, lysine (K) was used to replace the glutamic acid residue 164 (E164K) which is conserved in many animals (fly, zebrafish, mouse and human) and this E164K mutation recapitulated BNCH mutant phenotype. In conclusion, BNCH harboring E164K (BNCH*) was successfully produced by site-directed mutagenesis and cloned into pcDNA.3.1 vector. The construct was transformed into E. coli OmniMAX and that provides a valuable cell assay to search for the molecular ligand of BNCH. |
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| 653 | |aCloning |
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| 653 | |aBenchwarmer |
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| 653 | |aĐột Biến |
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| 653 | |aLysosomal membrane protein |
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| 653 | |aPlasmid pcDNA3.1 |
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| 690 | |aViện Kỹ thuật Công nghệ cao NTT |
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| 773 | |tTạp chí Khoa học và Công nghệ - Đại học Nguyễn Tất Thành |d2020|gtr. 06-11|x2615-9015|i12 |
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| 890 | |a0|b0|c1|d31 |
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