Your search keyword '"Sue-Hwa Lin"' showing total 5 results

1. The HIV-1 p6/EIAV p9 docking site in Alix is autoinhibited as revealed by a conformation-sensitive anti-Alix monoclonal antibody

Author

Sue Hwa Lin, Jian Kuang, Le Sun, Xi Zhou, Shujuan Pan, and Joe Corvera

Subjects

Protein Conformation, medicine.drug_class, Endosome, Viral protein, Immunoblotting, Gene Products, gag, Cell Cycle Proteins, Monoclonal antibody, medicine.disease_cause, gag Gene Products, Human Immunodeficiency Virus, Biochemistry, ESCRT, Virus, Cell Line, medicine, Humans, Immunoprecipitation, Molecular Biology, Binding Sites, Endosomal Sorting Complexes Required for Transport, biology, Calcium-Binding Proteins, HEK 293 cells, Antibodies, Monoclonal, Cell Biology, Molecular biology, Docking (molecular), HIV-1, biology.protein, Antibody, Infectious Anemia Virus, Equine, Protein Binding

Abstract

Alix [ALG-2 (apoptosis-linked gene 2)-interacting protein X], a component of the endosomal sorting machinery, contains a three-dimensional docking site for HIV-1 p6Gag or EIAV (equine infectious anaemia virus) p9Gag, and binding of the viral protein to this docking site allows the virus to hijack the host endosomal sorting machinery for budding from the plasma membrane. In the present study, we identified a monoclonal antibody that specifically recognizes the docking site for p6Gag/p9Gag and we used this antibody to probe the accessibility of the docking site in Alix. Our results show that the docking site is not available in cytosolic or recombinant Alix under native conditions and becomes available upon addition of the detergent Nonidet P40 or SDS. In HEK (human embryonic kidney)-293 cell lysates, an active p6Gag/p9Gag docking site is specifically available in Alix from the membrane fraction. The findings of the present study demonstrate that formation or exposure of the p6Gag/p9Gag docking site in Alix is a regulated event and that Alix association with the membrane may play a positive role in this process. Abbreviations: Alix, ALG-2 (apoptosis-linked gene 2)-interacting protein X; DOC, sodium deoxycholate; EIAV, equine infectious anaemia virus; ESCRT, endosomal sorting complex required for transport; GST, glutathione transferase; HA, haemagglutinin; HEK, human embryonic kidney; MVB, multivesicular body; MVE, multivesicular endosome; PRD, proline-rich region/domain; TBS, Tris-buffered saline

Published

2008

2. Differences in tissue-specific and embryonic expression of mouse Ceacam1 and Ceacam2 genes

Author

Eric HAN, Dillon PHAN, Piao LO, Matthew N. POY, Richard BEHRINGER, Sonia M. NAJJAR, and Sue-Hwa LIN

Subjects

Cell Biology, Molecular Biology, Biochemistry

Abstract

The intercellular adhesion molecule CEACAM1, also known as C-CAM1 (where CAM is cell-adhesion molecule), can function as a tumour suppressor in several carcinomas, including those of the prostate, breast, bladder and colon. This suggests that CEACAM1 may play an important role in the regulation of normal cell growth and differentiation. However, there is no direct evidence to support this putative function of CEACAM1. To elucidate its physiological function by targeted gene deletion, we isolated the Ceacam genes from a mouse 129 Sv/Ev library. Although there is only one Ceacam1 gene in humans and one in rats, two homologous genes (Ceacam1 and Ceacam2) have been identified in the mouse. Our sequence analysis revealed that the genes encoded nine exons and spanned approx. 16-17 kb (Ceacam1) and 25kb (Ceacam2). The genes were highly similar (79.6%). The major differences in the protein-coding regions were located in exons 2, 5 and 6 (76.9%, 87.0% and 78.5% similarity respectively). In addition, introns 2, 5 and 7 were also significantly different, being 29.7%, 59.8% and 64.5% similar respectively. While most of these differences were due to nucleotide substitutions, two insertions of 418 and 5849bp occurred in intron 2 of Ceacam2, and another two insertions of 1384 and 197bp occurred in introns 5 and 7 respectively. To determine whether functional redundancy exists between Ceacam1 and Ceacam2, we examined their expression in 16 mouse tissues by using semi-quantitative reverse transcription-PCR. As in human and rat, in the mouse Ceacam1 mRNA was highly abundant in the liver, small intestine, prostate and spleen. In contrast, Ceacam2 mRNA was only detected in kidney, testis and, to a lesser extent, spleen. Reverse transcription-PCR using testis RNA indicated that Ceacam2 in the testis is an alternatively spliced form containing only exons 1, 2, 5, 6, 8 and 9. In the mouse embryo, Ceacam1 mRNA was detected at day 8.5, disappeared between days 9.5 and 12.5, and re-appeared at day 19. On the other hand, no Ceacam2 mRNA was detected throughout embryonic development. The different tissue expression patterns and regulation during embryonic development suggest that the CEACAM1 and CEACAM2 proteins, although highly similar, may have different functions both during mouse development and in adulthood. The Ceacam1 and Ceacam2 sequences have been deposited in the GenBank®/EMBL/DDBJ/GSDB Nucleotide Sequence Databases with accession numbers AF287911 and AF287912 respectively.

Published

2001

3. Functional expression of a human thrombin receptor in Sf9 insect cells: evidence for an active tethered ligand

Author

Weiping Luo, William P. Schilling, Sue Hwa Lin, Karen Earley, and Xilin Chen

Subjects

DNA, Complementary, Molecular Sequence Data, Thermolysin, Hirudin, Sf9, Stimulation, Spodoptera, Ligands, Aminopeptidases, Biochemistry, Thrombin, Homologous desensitization, Endopeptidases, Thrombin receptor, Tumor Cells, Cultured, medicine, Animals, Humans, Methionyl Aminopeptidases, Amino Acid Sequence, Cloning, Molecular, Receptor, Molecular Biology, Base Sequence, Chemistry, Cell Biology, Molecular biology, Peptide Fragments, Calcium, Receptors, Thrombin, Research Article, medicine.drug

Abstract

Desensitization of recombinant human thrombin receptors expressed in Sf9 insect cells was compared with native thrombin receptors in megakaryoblast erythroleukaemia (HEL) cells. Addition of thrombin (2 units/ml) or agonist peptide SFLLRN (10 microM) to HEL cells, or to Sf9 cells infected with recombinant baculovirus containing the thrombin receptor cDNA, produced an increase in the free cytosolic Ca2+ concentration ([Ca2+]i) as measured by fura-2. The response in HEL cells was transient, reflecting a rapid homologous desensitization. In contrast, [Ca2+]i in Sf9 cells expressing the thrombin receptor increased rapidly to a peak value that slowly declined, but remained elevated for at least 12 min following stimulation by thrombin. The sustained [Ca2+]i response to thrombin was not reversed by washout of thrombin or by any subsequent addition of hirudin. Pretreatment of Sf9 cells with either thrombin (2 units/ml) or SFLLRN (10 or 50 microM) for 5 min produced a shift in the ED50 for SFLLRN (added 10 min after washout) from 0.4 microM to 20 and 7 microM, respectively. Thus, desensitization of thrombin receptors expressed in Sf9 cells occurs slowly and reflects a decrease in receptor affinity. The sustained [Ca2+]i response in Sf9 cells stimulated by thrombin may reflect continuous activation by the tethered ligand. To test this hypothesis, the effect of protease treatment during the sustained phase of the response was examined. Addition of either aminopeptidase M or thermolysin reversed the sustained response to SFLLRN, but only thermolysin reversed the sustained response to thrombin. Thermolysin had no effect on the change in [Ca2+]i observed following carbachol stimulation of Sf9 cells expressing the M5 muscarinic receptor. Furthermore, following thermolysin treatment, the cells remained responsive to a subsequent application of SFLLRN. These results demonstrate that the tethered ligand remains active for extended periods of time after thrombin stimulation and suggests that further hydrolysis by extracellular proteases may represent an important mechanism of rapid receptor deactivation.

Published

1996

4. The CHMP4b- and Src-docking sites in the Bro1 domain are autoinhibited in the native state of Alix.

Author

Xi Zhou, Shujuan Pan, Le Sun, Joe Corvera, Yu-Chen Lee, Sue-Hwa Lin, and Jian Kuang

Subjects

BINDING sites, RECOMBINANT proteins, PROTEIN-tyrosine kinases, APOPTOSIS, DETERGENTS, BIOCHEMISTRY

Abstract

The Bro1 domain of Alix [ALG-2 (apoptosis-linked gene 2)-interacting protein X], which plays important roles in endosomal sorting and multiple ESCRT (endosomal sorting complex required for transport)-linked processes, contains the docking sites for the ESCRT-III component CHMP4b (charged multivesicular body protein 4b) and the regulatory tyrosine kinase, Src. Although the structural bases for these docking sites have been defined by crystallography studies, it has not been determined whether these sites are available in the native state of Alix. In the present study, we demonstrate that these two docking sites are unavailable in recombinant Alix under native conditions and that their availabilities can be induced by detergents. In HEK (human embryonic kidney)-293 cell lysates, these two docking sites are not available in cytosolic Alix, but are available in membrane-bound Alix. These findings show that the native state of Alix does not have a functional Bro1 domain and predict that Alix's involvement in endosomal sorting and other ESCRT-linked processes requires an activation step that relieves the autoinhibition of the Bro1 domain. [ABSTRACT FROM AUTHOR]

Published

2009

5. The HIV-1 p6/EIAV p9 docking site in Alix is autoinhibited as revealed by a conformation-sensitive anti-Alix monoclonal antibody.

Author

Xi Zhou, Shujuan Pan, Le Sun, Joe Corvera, Sue-Hwa Lin, and Jian Kuang

Subjects

PROTEIN binding, MONOCLONAL antibodies, HIV, IMMUNOGLOBULINS, CELL membranes

Abstract

Alix [ALG-2 (apoptosis-linked gene 2)-interacting protein X], a component of the endosomal sorting machinery, contains a three-dimensional docking site for HIV-1 p6Gag or EIAV (equine infectious anaemia virus) p9Gag, and binding of the viral protein to this docking site allows the virus to hijack the host endosomal sorting machinery for budding from the plasma membrane. In the present study, we identified a monoclonal antibody that specifically recognizes the docking site for p6Gag/p9Gag and we used this antibody to probe the accessibility of the docking site in Alix. Our results show that the docking site is not available in cytosolic or recombinant Alix under native conditions and becomes available upon addition of the detergent Nonidet P40 or SDS. In HEK (human embryonic kidney)-293 cell lysates, an active p6Gag/p9Gag docking site is specifically available in Alix from the membrane fraction. The findings of the present study demonstrate that formation or exposure of the p6Gag/p9Gag docking site in Alix is a regulated event and that Alix association with the membrane may play a positive role in this process. [ABSTRACT FROM AUTHOR]

Published

2008