rabies pathogenesis
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2020 ◽  
Author(s):  
Fatemeh Zandi ◽  
Vahid Khalaj ◽  
Fatemeh Goshadrou ◽  
Anna Meyfour ◽  
Alireza Gholami ◽  
...  

Abstract Multifunctional matrix protein (M) of rabies virus (RABV) plays essential roles in the pathogenesis of rabies infection. Identification of M protein interacting partners in target hosts could help to elucidate the biological pathways and molecular mechanisms involved in the pathogenesis of this virus. In this study, two-dimensional Far-western blotting (2D-Far-WB) technique was applied to find possible matrix protein partners in the rat brainstem. Recombinant RABV M was expressed in Pichia pastoris (P. pastoris) and was partially purified. Subsequently, 2D-Far-WB determined six rat brainstem proteins interacted with recombinant M protein which were identified by mass spectrometry. Functional annotation by gene ontology analysis determined these proteins were involved in the regulation of synaptic transmission processes, metabolic process, and cell morphogenesis-cytoskeleton organization. The interaction of viral M protein with selected host proteins in mouse Neuro-2a cells infected with RABV was verified by super-resolution confocal microscopy. Molecular docking simulations also demonstrated the formation of RABV M complexes. However, further confirmation with co-immunoprecipitation (Co-IP), was only successful for M-actin cytoplasmic1 interaction. Totally, our study revealed actin cytoplasmic1 as a binding partner of M protein, which might have important role(s) in rabies pathogenesis.


Viruses ◽  
2020 ◽  
Vol 12 (9) ◽  
pp. 914
Author(s):  
Tatsuki Takahashi ◽  
Maho Inukai ◽  
Michihito Sasaki ◽  
Madlin Potratz ◽  
Supasiri Jarusombuti ◽  
...  

The rabies virus strain Komatsugawa (Koma), which was isolated from a dog in Tokyo in the 1940s before eradication of rabies in Japan in 1957, is known as the only existent Japanese field strain (street strain). Although this strain potentially provides a useful model to study rabies pathogenesis, little is known about its genetic and phenotypic properties. Notably, this strain underwent serial passages in rodents after isolation, indicating the possibility that it may have lost biological characteristics as a street strain. In this study, to evaluate the utility of the Koma strain for studying rabies pathogenesis, we examined the genetic properties and in vitro and in vivo phenotypes. Genome-wide genetic analyses showed that, consistent with previous findings from partial sequence analyses, the Koma strain is closely related to a Russian street strain within the Arctic-related phylogenetic clade. Phenotypic examinations in vitro revealed that the Koma strain and the representative street strains are less neurotropic than the laboratory strains. Examination by using a mouse model demonstrated that the Koma strain and the street strains are more neuroinvasive than the laboratory strains. These findings indicate that the Koma strain retains phenotypes similar to those of street strains, and is therefore useful for studying rabies pathogenesis.


Viruses ◽  
2020 ◽  
Vol 12 (4) ◽  
pp. 359 ◽  
Author(s):  
Vinod Sundaramoorthy ◽  
Nathan Godde ◽  
Ryan J. Farr ◽  
Diane Green ◽  
John M. Haynes ◽  
...  

Rabies is a zoonotic neurological infection caused by lyssavirus that continues to result in devastating loss of human life. Many aspects of rabies pathogenesis in human neurons are not well understood. Lack of appropriate ex-vivo models for studying rabies infection in human neurons has contributed to this knowledge gap. In this study, we utilize advances in stem cell technology to characterize rabies infection in human stem cell-derived neurons. We show key cellular features of rabies infection in our human neural cultures, including upregulation of inflammatory chemokines, lack of neuronal apoptosis, and axonal transmission of viruses in neuronal networks. In addition, we highlight specific differences in cellular pathogenesis between laboratory-adapted and field strain lyssavirus. This study therefore defines the first stem cell-derived ex-vivo model system to study rabies pathogenesis in human neurons. This new model system demonstrates the potential for enabling an increased understanding of molecular mechanisms in human rabies, which could lead to improved control methods.


2018 ◽  
Vol 37 (2) ◽  
pp. 323-330 ◽  
Author(s):  
A.C. BANYARD ◽  
N. TORDO
Keyword(s):  

Author(s):  
Alan C. Jackson

Rabies is an acute viral infection involving the central nervous system with distinctive clinical features reflecting early brainstem involvement, including hydrophobia. This infection is usually transmitted by animal bites, typically from dogs or wildlife, including bats. There is a progressive clinical course to coma and the disease is virtually always fatal. When rabies is treated aggressively there are usually multiple medical complications, including multiple organ failure. Therapeutic attempts have been disappointing and new approaches need to be taken in the future. An improved understanding of rabies pathogenesis might lead to important insights into the development of new therapeutic approaches.


2002 ◽  
Vol 8 (4) ◽  
pp. 267-269 ◽  
Author(s):  
Alan C Jackson
Keyword(s):  

Author(s):  
Alan C. Jackson

Rabies is an important disease in wildlife in the United States and Canada, and dog rabies is still a major public health problem in many developing countries of the world. Rabies virus is transmitted in saliva by animal bites. Bats transmitted most recent cases of human rabies in the United States, often without known exposures. There have been recent developments in our understanding of rabies pathogenesis. Characteristic clinical features should raise the possibility of a diagnosis of rabies and initiation of appropriate diagnostic tests. Therapy of human rabies has been futile except in four patients who were immunized with rabies vaccine prior to the onset of their disease. Rabies can be prevented after an exposure in unimmunized patients with local wound cleansing and administration of rabies vaccine and human rabies immune globulin.


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