Template:Viral life cycle Viral shedding refers to the successful production of virus progeny and that the progeny is leaving the cell to infect other host cells. Once replication has been completed and the host cell is exhausted of all resources in making viral progeny, the viruses may begin to leave the cell by several methods.
The term is used to refer to shedding from a single cell, shedding from one part of the body into another part of the body, and shedding from bodies into the environment where the viruses may infect other bodies.
"Budding" through the cell envelope, in effect using the cell's membrane for the virus itself is most effective for viruses that need an envelope in the first place. These include enveloped viruses such as HSV, SARS or smallpox. Prior to budding, the virus may put its own receptor onto the surface of the cell in preparation for the virus to bud through, forming an envelope with the viral receptors already on it. This process will slowly use up the cell membrane and eventually lead to the demise of the cell. This is also how antiviral responses are able to detect virus infected cells.
By forcing the cell to undergo apoptosis or cell suicide, release of progeny into the extracellular space is possible. However, apoptosis does not necessarily result in the cell simply popping open, spilling its contents into the extracellular space. Rather, apoptosis is usually controlled and results in the cell's genome being chopped up, before apoptotitic bodies of dead cell material clump off the cell to be absorbed by macrophages. This is a good way for a virus to get into macrophages either to infect them or simply travel to other tissues in the body. Although this process is primarily used by non-enveloped viruses, enveloped viruses may also use this. HIV is an example of an enveloped virus that exhibits this process for the infection of macrophages.
Via reverse endocytosis
It may not be in a virus's best interest to kill the cell in order to escape it for further infection of other host cells. It is then reverse endocytotic release of viral progeny is used to release viral particles. Viral progeny are synthesized within the cell and the host cell's transport system is used to enclose vacuoles of virus progeny for release into the extracellular space. This is used primarily by non-enveloped viruses, although enveloped viruses display this too. An example is the use of recycling viral particle receptors in the enveloped varicella-zoster virus.
- ↑ N.J. Dimmock et al. "Introduction to Modern Virology, 6th edition." Blackwell Publishing, 2007.
- ↑  Massachusetts Department of Public Health - Rabies Control Plan - CHAPTER 1: GENERAL INFORMATION - "Definitions as Used in this Document [...] Shedding - The release of rabies virus from the salivary glands into the saliva."
- ↑ J Infect Dis. 1979 Oct;140(4):610-3 article Viral shedding patterns of children with influenza B infection
- ↑ Owen Pornillos, Jennifer E. Garrus and Wesley I. Sundquist. "Mechanisms of enveloped RNA virus budding." Trends in Cell Biology, Volume 12, Issue 12, 1 December 2002, Pages 569-579
- ↑ Sheila A. Stewart, Betty Poon, Joo Y. Song, and Irvin S. Y. Chen. "Human Immunodeficiency Virus Type 1 Vpr Induces Apoptosis through Caspase Activation." Journal of Virology, April 2000, p. 3105-3111, Vol. 74, No. 7
- ↑ J K Olson and C Grose. "Endocytosis and recycling of varicella-zoster virus Fc receptor glycoprotein gE: internalization mediated by a YXXL motif in the cytoplasmic tail." J Virol. 1997 May; 71(5): 4042–4054.