Your search keyword '"Anaplasma ovis metabolism"' showing total 3 results

1. Identification and evaluation of midgut protein RL12 of Dermacentor silvarum interacting with Anaplasma ovis VirD4.

Author

Iqbal N, Mukhtar MU, Yang J, Niu Q, Li Z, Zhao S, Zhao Y, Guan G, Liu Z, and Yin H

Subjects

Anaplasma ovis metabolism, Animals, Arachnid Vectors metabolism, Arachnid Vectors microbiology, Arthropod Proteins metabolism, Bacterial Proteins metabolism, Dermacentor metabolism, Dermacentor microbiology, Digestive System metabolism, Digestive System microbiology, Ribosomal Proteins metabolism, Anaplasma ovis genetics, Arachnid Vectors genetics, Arthropod Proteins genetics, Bacterial Proteins genetics, Dermacentor genetics, Ribosomal Proteins genetics

Abstract

Anaplasma ovis, a tick-borne intra-erythrocytic Gram-negative bacterium, is a causative agent of ovine anaplasmosis. It is known that Dermacentor ticks act as biological vectors for A. ovis. VirD4 is the machine component of Type IV Secretion System of A. ovis. To better understand the pathogen-vector interaction, VirD4 was used as a bait protein for screening midgut proteins of Dermacentor silvarum via yeast two-hybrid mating assay. As a result, a ribosomal protein RL12 was identified from the midgut cDNA library of D. silvarum. For further validation, using in vitro Glutathione S-transferase (GST) pull-down assay, interaction between the proteins, GST-RL12 and HIS-VirD4, was observed in Western blot analysis. The study is first of its kind reporting a D. silvarum midgut protein interaction with VirD4 from A. ovis. Functional annotations showed some important cellular processes are attributed to the protein, particularly in the stringent response and biogenesis. The results of the study suggest the involvement of the VirD4-RL12 interaction in the regulation of signaling pathways, which is a tool for understanding the pathogen-vector interaction., (Copyright © 2021 Elsevier GmbH. All rights reserved.)

Published

2021

2. Identification and evaluation of UL36 protein from Dermacentor silvarum salivary gland and its interaction with Anaplasma ovis VirB10.

Author

Mukhtar MU, Iqbal N, Yang J, Niu Q, Zhao S, Li Z, Zhao Y, Rashid M, Chen Z, Guan G, Liu Z, and Yin H

Subjects

Anaplasma ovis genetics, Animals, Arthropod Proteins genetics, Bacterial Proteins genetics, Dermacentor genetics, Host-Parasite Interactions, Protein Binding, Salivary Glands metabolism, Salivary Glands microbiology, Two-Hybrid System Techniques, Type IV Secretion Systems genetics, Anaplasma ovis metabolism, Arthropod Proteins metabolism, Bacterial Proteins metabolism, Dermacentor metabolism, Dermacentor microbiology, Type IV Secretion Systems metabolism

Abstract

Background: Anaplasma ovis is a gram-negative, tick-borne obligate intraerythrocytic pathogen, which causes ovine anaplasmosis in small ruminants worldwide. VirB10 of A. ovis is an integral component of the Type IV Secretion System (T4SS). The T4SS is used by bacteria to transfer DNA and/or proteins undeviatingly into the host cell to increase their virulence. To more thoroughly understand the interaction between A. ovis and Dermacentor silvarum, a vector containing the virb10 gene of A. ovis was used as a bait plasmid to screen interacting proteins from the cDNA library of the D. silvarum salivary gland using the yeast two-hybrid system., Methods: The cDNA of the D. silvarum salivary gland was cloned into the pGADT7-SmaI vector (prey plasmid) to construct the yeast two-hybrid cDNA library. The virb10 gene was cloned into the pGBKT7 vector to generate a bait plasmid. Any gene auto-activation or toxicity effects in the yeast strain Y2HGold were excluded. The screening was performed by combining the bait and prey plasmids in yeast strains to identify positive preys. The positive preys were then sequenced, and the obtained sequences were subjected to further analyses using Gene Ontology, UniProt, SMART, and STRING. Additionally, the interaction between the bait and the prey was evaluated using the glutathione S-transferase (GST) pull-down assay., Results: A total of two clones were obtained from the cDNA library using the yeast two-hybrid system, and the sequence analysis showed that both clones encoded the same large tegument protein, UL36. Furthermore, the proteins GST-UL36 and His-VirB10 were successfully expressed in vitro and the interaction between the two proteins was successfully demonstrated by the GST pull-down assay., Conclusions: To our knowledge, this study is the first to screen for D. silvarum salivary gland proteins that interact with A. ovis VirB10. The resulting candidate, UL36, is a multi-functional protein. Further investigations into the functionality of UL36 should be carried out, which might help in identifying novel prevention and treatment strategies for A. ovis infection. The present study provides a base for exploring and further understanding the interactions between A. ovis and D. silvarum.

Published

2020

3. Anaplasma ovis as the suspected cause of mortality in a neonatal elk calf.

Author

Hendrix GK, Brayton KA, and Burcham GN

Subjects

Amino Acid Sequence, Anaplasma ovis metabolism, Anaplasmosis microbiology, Animals, Animals, Newborn, Bacterial Proteins chemistry, Indiana, Membrane Proteins chemistry, Polymerase Chain Reaction veterinary, Anaplasma ovis genetics, Anaplasmosis diagnosis, Bacterial Proteins genetics, Deer, Membrane Proteins genetics

Abstract

Anaplasma ovis infection is known to occur in elk experimentally, but without clinical signs or significant clinicopathologic changes. An elk farm in southern Indiana experienced the death of 3 neonates. Gross findings suggested hemolytic anemia as the cause of death. Splenic impression smears revealed numerous intra-erythrocytic parasites compatible with Anaplasma spp. Products of a semi-nested PCR targeting the msp4 gene of A. ovis were sequenced and had 100% identity with published A. ovis sequences. Given the clinical presentation, vertical transmission of A. ovis was suspected. Pathologic and molecular findings confirmed that natural A. ovis infection occurred in an elk calf.

Published

2019