Your search keyword '"Mohammed Al Balushi"' showing total 2 results

1. Peptide-receptive Major Histocompatibility Complex Class I Molecules Cycle between Endoplasmic Reticulum and cis-Golgi in Wild-type Lymphocytes.

Author

Garstka, Malgorzata, Borchert, Britta, Mohammed Al-Balushi, Praveen, P. V. K., Kühl, Nicole, Majoul, Irma, Duden, Rainer, and Springer, Sebastian

Subjects

*HLA histocompatibility antigens, *MAJOR histocompatibility complex, *TRANSPLANTATION immunology, *CHEMICAL reactions, *BIOMOLECULES, *LIFE sciences, *BIOCHEMISTRY

Abstract

Prior to binding to a high affinity peptide and transporting it to the cell surface, major histocompatibility complex class I molecules are retained inside the cell by retention in the endoplasmic retlculum (ER), recycling through the ER-Golgi intermediate compartment and possibly the cis-Golgi, or both. Using fluorescence microscopy and a novel in vitro COPII (ER-to-ERGolgi intermediate compartment) vesicle formation assay, we find that in both lymphocytes and fibroblasts that lack the functional transporter associated with antigen presentation, class I molecules exit the ER and reach the cis-Golgi. Intriguingly, in wild-type T1 lymphoma cells, peptide-occupied and peptidereceptive class I molecules are simultaneously exported from ER membranes with similar efficiencies. Our results suggest that binding of high affinity peptide and exit from the ER are not coupled, that the major histocompatibility complex class I qualitycontrol compartment extends into the Golgi apparatus under standard conditions, and that peptide loading onto class I molecules may occur in post-ER compartments. [ABSTRACT FROM AUTHOR]

Published

2007

2. A genome-led study on the pathogenesis of Fusobacterium necrophorum infections.

Author

Thapa, Gary, Jayal, Ambikesh, Sikazwe, Elvis, Perry, Thomas, Mohammed Al Balushi, Ali, and Livingstone, Paul

Subjects

*FUSOBACTERIUM, *WHOLE genome sequencing, *PATHOGENESIS, *SEQUENCE analysis

Abstract

• Fusobacterium necrophorum causes a wide range of invasive and non-invasive infections. • Genome sequence analysis gives an overview of the pathogenic mechanisms involved in F. necrophorum infections. • Phylogenomics of human isolates shows no grouping relevant to their clinical features, although animal isolates are grouped separately. • Virulome reveals marker genes that can be used for diagnostic and therapeutic purposes. Fusobacterium necrophorum causes a range of mild to life threatening infections and there is uncertainty in terms of diagnosis and treatment due to the lack of knowledge on their pathogenic mechanisms. This study characterised genomes of F. necrophorum to compare their virulence factors and investigate potential infection markers. 27 isolates of F. necrophorum from patients with pharyngotonsillitis were subjected to whole genome sequencing and compared with 42 genomes published in the NCBI database. Phylogenomics, pangemome, pan-GWAS and virulome were analysed to study strain variations with reference to virulence factors. Core genome based phylogenomic tree exhibited three clades of which Clade A belonged to F. necrophorum subsp necrophorum , clades B and C were F. necrophorum subsp funduliforme. Pan-GWAS and Pan-Virulome suggest some marker genes associated with clinical sources of isolation that needs further validation. Our study highlights some interesting features of the pathogenesis of F. necrophorum infections. Although the animal isolate genomes had some marker genes, the genomes of human isolates did not exhibit clear correlation to their clinical sources of isolation. This prompts to think of other mechanisms such as co-infections or host factors that can be involved in the pathogenesis. [ABSTRACT FROM AUTHOR]

Published

2022