Non-Polio enterovirus infections pathophysiology: Difference between revisions

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==Pathophysiology==
==Pathophysiology==
===[[Non-polio]] [[non-rhinovirus]] [[enteroviruses]]===
===[[Non-polio]] [[non-rhinovirus]] [[enteroviruses]]===
* Replicate in the [[oropharyngeal]] [[mucosa]] and the [[intestines]], leading to their detection in [[oral]] [[secretions]] and [[stool]], the latter showing evidence of the [[pathogen]] months after resolution of the [[symptoms]].
* Targets the [[lymphatic]] [[tissues]] such as the [[Peyer's patches]] and the [[tonsils]], paving the way for [[lymphatic]] and [[hematogenous]] [[dissemination]]
* Manifestations include [[myocarditis]], [[pancreatitis]] and often a second, stronger [[viremia]]. This can cause  serious clinical illness and facilitate direct crossing of the [[blood-brain]] barrier to affect the [[central nervous system]].
* Alternative mechanisms include a "Trojan horse"entry model mediated by [[virus-infected]] [[leukocytes]].
*Once present in the [[CNS]], persistent [[infection]] is possible, likely by an [[immune]] response to the [[apoptosis]] and [[autophagy]] induced by this group of [[viruses]].
===[[Rhinoviruses]]===
===[[Rhinoviruses]]===
== References ==
== References ==

Revision as of 18:36, 4 February 2023

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Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1] Associate Editor(s)-in-Chief: {Sujaya}}

Overview

The cellular uptake of enteorviruses is mediated by receptor molecules such as, intracellular adhesion molecule-1 (ICAM-1), low-density lipoprotein receptor (LDL-R), and non-protein factors such as heparan sulfate and sialic acid. Incubation periods range from 12 hours to 5 days, with experimental volunteers reporting symptoms several hours after aritficial inoculation.

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Non-polio non-rhinovirus enteroviruses

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