Tick-borne encephalitis pathophysiology: Difference between revisions

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Revision as of 21:13, 9 March 2016

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1] Associate Editor(s)-in-Chief: Ilan Dock, B.S.

Overview

Tick-borne encephalitis is caused by a (+) ssRNA virus of the Flavivirus genus. Three subtypes of the virus exist including the Far East, European, and Siberian subtypes. The Ixodidae family of ticks is the primary vector associated with transmission, with other modes of transmission including the consumption of unpasteurized, raw milk.^[1] Pathogenesis occurs as the virus binds to a host cell receptor. Through a series of reactions, the virus enters the cell, is translated, and hi-jacks the host cell's replication machinery. After which immature virions are released within the cell, to ultimately spread infection. Viral replication will often occur within subcutaneous tissue. Replication also occurs within the lymph nodes, causing immense damage to the immune system. A later phase of the virus results in an infection of the CNS as the immune response increases the permeability of the blood-brain barrier. ^[2]

Transmission

The Ixodidae family of hard ticks have been reported as the vector and reservoir of the Tick-borne encephalitis virus.
Other modes of transmission include the consumption of raw milk as well as vertical transmission from mother to fetus. ^[1]

Virology

Member of the Falvivirus genus
Flaviviridae family
Three subtypes: Far East, European, and Siberian
Viral strains are mostly homogeneous within infected European tick populations.
Diversity exists within viral strains carried by Siberian and Far Eastern tick populations. Thus these populations host antigenic variations and a variety of subtypes.
However the antigenic similarity within these populations allows for a generalized protection method among the different subtypes. ^[2]

Genomics

(+)ssRNA genome enclosed in a capsid protein.
Genome is protected by a lipid bilayer, provided by the host or target cell.
Virus's physical attributes include a spherical particle with an approximate diameter of 50-60nm.
The genome lacks a 3'-poly(A) tail, yet provides a 5' cap.
In terms of length, the genome spans an average of 11kb.^[2]

Pathogenesis

The process begins as the virus binds to a host cell receptor.
A host cell will internalize the virus using endocytosis.
Post-endocytosis, acidification of the viral envelope causes conformation changes of the E protein, resulting in the attachment of the viral envelope to a endosomal vesicle.
Once properly mounted on the endosomal vesicle, the viral envelope will release the viral nucleocapsid into the surrounding cytoplasm.
Translation of the virus yields a 3414 amino acid long polyprotein.
The polyprotein is cleaved by both cellular and viral proteases.
The cleaving process results in three structural proteins called C, prM, and E as well as seven non-structural proteins.^[2]
The C protein forms a virion nucleocapsid through binding to viral DNA.
The E protein is necessary as a ligand to cell receptors and as a fusion protein.
The other non-structural proteins serve as proteases, polymerases, complement binding antigens, or function within the replication process.
Finally the processes concludes as the positive-stranded genome is translated while the negative-strand of RNA provides grounds for the RNA replication process.
Assembly of the virus occurs within the endoplasmic reticulum.
Post-assembly immature virions are released within the cell.^[2]

Schematic drawing of the steps during TBE virus infection. (1) TBE virus transmission from an infected tick, (2) TBE virus replication in regional lymph nodes, (3) primary viremia, (4) replication of the virus in other organs and tissues, (5) secondary viremia, (6) TBE virus crossing of the blood-brain barrier, and (7) virus infection of the brain^[2]]]

Viral pathway within a mammalian host

Virus replication commonly occurs within subcutaneous tissue.
Dendritic cells transport the virus to the lymph nodes.
The virus replicates at a high rate within the lymph nodes, further travelling into the bloodstream.
Lymphocytes suffer great reductions due to infection with the regional lymph nodes.
Further infection of external tissues occur within the viremic phase
The later phase results in the infection of the CNS.
Furthermore a host's immune system will add to the severity of the infection, as resulting immune response includes inflammation CD8+ T-cells infiltrating the brain.
Other immune responses such as the upregulation of proinflammatory cytokines increase the permeability of the blood-brain barrier.^[2]

References

↑ ^1.0 ^1.1 Tick-borne encephalitis transmission. http://www.cdc.gov/vhf/tbe/transmission/index.html Accessed February 5, 2016.
↑ ^2.0 ^2.1 ^2.2 ^2.3 ^2.4 ^2.5 ^2.6 Tick-borne Encephalitis Virus: A General Overview. http://cdn.intechopen.com/pdfs-wm/20866.pdf. Accessed February 4, 2016.

[Trans_CDC-1] 1.0 ^1.1 Tick-borne encephalitis transmission. http://www.cdc.gov/vhf/tbe/transmission/index.html Accessed February 5, 2016.

[Enceph_Prime-2] 2.0 ^2.1 ^2.2 ^2.3 ^2.4 ^2.5 ^2.6 Tick-borne Encephalitis Virus: A General Overview. http://cdn.intechopen.com/pdfs-wm/20866.pdf. Accessed February 4, 2016.

[1]

[2]

@@ Line 4: / Line 4: @@
 ==Overview==
-Tick-borne encephalitis is caused by a (+) ssRNA virus of the Flavivirus genus. Three subtypes of the virus exist including the Far East, European, and Siberian subtypes. The Ixodidae family of ticks is the primary vector associated with transmission, with other modes of transmission including the consumption of unpasteurized, raw milk.<ref name="Trans CDC">Tick-borne encephalitis transmission. http://www.cdc.gov/vhf/tbe/transmission/index.html Accessed February 5, 2016. </ref> Pathogenesis occurs as the virus binds to a host cell receptor. Through a series of reactions, the virus enters the cell, is translated, and hi-jacks the host cell's replication machinery. After which immature virions are released within the cell, to ultimately spread infection. Viral replication will often occur within subcutaneous tissue. Replication also occurs within the lymph nodes, causing immense damage to the immune system. A later phase of the virus results in an infection of the CNS as the immune response increases the  permeability of the blood-brain barrier. <ref name="Enceph Prime">Tick-borne Encephalitis Virus: A General Overview. http://cdn.intechopen.com/pdfs-wm/20866.pdf. Accessed February 4, 2016. </ref>
+Tick-borne encephalitis is caused by a (+) ssRNA virus of the [[Flavivirus]] genus. Three subtypes of the virus exist including the Far East, European, and Siberian subtypes. The [[Ixodidae]] family of ticks is the primary [[vector]] associated with [[transmission]], with other modes of [[transmission]] including the consumption of unpasteurized, raw milk.<ref name="Trans CDC">Tick-borne encephalitis transmission. http://www.cdc.gov/vhf/tbe/transmission/index.html Accessed February 5, 2016. </ref> [[Pathogenesis]] occurs as the [[virus]] binds to a host cell receptor. Through a series of reactions, the [[virus]] enters the cell, is translated, and hi-jacks the host cell's replication machinery. After which immature [[virions]] are released within the cell, to ultimately spread infection. Viral [[replication]] will often occur within [[subcutaneous tissue]]. Replication also occurs within the [[lymph nodes]], causing immense damage to the [[immune system]]. A later phase of the virus results in an infection of the [[CNS]] as the [[immune response]] increases the  [[permeability]] of the [[blood-brain barrier]]. <ref name="Enceph Prime">Tick-borne Encephalitis Virus: A General Overview. http://cdn.intechopen.com/pdfs-wm/20866.pdf. Accessed February 4, 2016. </ref>
 ==Transmission==
-*The ''Ixodidae'' family of hard ticks have been reported as the vector and reservoir of the Tick-borne encephalitis virus.
+*The ''[[Ixodidae]]'' family of hard ticks have been reported as the [[vector]] and reservoir of the Tick-borne encephalitis virus.
-*Other modes of transmission include the consumption of raw milk as well as vertical transmission from mother to fetus. <ref name="Trans CDC">Tick-borne encephalitis transmission. http://www.cdc.gov/vhf/tbe/transmission/index.html Accessed February 5, 2016. </ref>
+*Other modes of [[transmission]] include the consumption of raw milk as well as vertical transmission from mother to fetus. <ref name="Trans CDC">Tick-borne encephalitis transmission. http://www.cdc.gov/vhf/tbe/transmission/index.html Accessed February 5, 2016. </ref>
 ==Virology==
 *Member of the Falvivirus genus
-*Flaviviridae family
+*[[Flaviviridae]] family
 *Three subtypes: Far East, European, and Siberian
-*Viral strains are mostly homogeneous within infected European tick populations.
+*Viral [[strains]] are mostly homogeneous within infected European tick populations.
 *Diversity exists within viral strains carried by Siberian and Far Eastern tick populations. Thus these populations host antigenic variations and a variety of subtypes.
-*However the antigenic similarity within these populations allows for a generalized protection method among the different subtypes. <ref name="Enceph Prime">Tick-borne Encephalitis Virus: A General Overview. http://cdn.intechopen.com/pdfs-wm/20866.pdf. Accessed February 4, 2016. </ref>
+*However the [[antigenic]] similarity within these populations allows for a generalized protection method among the different subtypes. <ref name="Enceph Prime">Tick-borne Encephalitis Virus: A General Overview. http://cdn.intechopen.com/pdfs-wm/20866.pdf. Accessed February 4, 2016. </ref>
 ===Genomics===
-*(+)ssRNA genome enclosed in a capsid protein.
+*(+)ssRNA genome enclosed in a [[capsid]] protein.
-*Genome is protected by a lipid bilayer, provided by the host or target cell.
+*Genome is protected by a [[lipid bilayer]], provided by the host or target cell.
 *Virus's physical attributes include a spherical particle with an approximate diameter of 50-60nm.
 *The genome lacks a 3'-poly(A) tail, yet provides a 5' cap.
@@ Line 28: / Line 28: @@
 *The process begins as the virus binds to a host cell receptor.
-*A host cell will internalize the virus using endocytosis.
+*A host cell will internalize the virus using [[endocytosis]].
-*Post-endocytosis, acidification of the viral envelope causes conformation changes of the E protein, resulting in the attachment of the viral envelope to a endosomal vesicle.
+*Post-[[endocytosis]], acidification of the viral envelope causes conformation changes of the E protein, resulting in the attachment of the viral envelope to a [[Endosomal membrane|endosomal]] vesicle.
-*Once properly mounted on the endosomal vesicle, the viral envelope will release the viral nucleocapsid into the surrounding cytoplasm.
+*Once properly mounted on the [[Endosome|endosomal]] vesicle, the viral envelope will release the viral [[nucleocapsid]] into the surrounding [[cytoplasm]].
-*Translation of the virus yields a 3414 amino acid long polyprotein.
+*Translation of the virus yields a 3414 amino acid long [[polyprotein]].
-*The polyprotein is cleaved by both cellular and viral proteases.
+*The [[polyprotein]] is cleaved by both cellular and viral [[proteases]].
-*The cleaving process results in three structural proteins called C, prM, and E as well as seven non-structural proteins.<ref name="Enceph Prime">Tick-borne Encephalitis Virus: A General Overview. http://cdn.intechopen.com/pdfs-wm/20866.pdf. Accessed February 4, 2016. </ref>
+*The cleaving process results in three structural [[proteins]] called C, prM, and E as well as seven non-structural proteins.<ref name="Enceph Prime">Tick-borne Encephalitis Virus: A General Overview. http://cdn.intechopen.com/pdfs-wm/20866.pdf. Accessed February 4, 2016. </ref>
-*The C protein forms a virion nucleocapsid through binding to viral DNA.
+*The C protein forms a [[virion]] [[nucleocapsid]] through binding to viral DNA.
-*The E protein is necessary as a ligand to cell receptors and as a fusion protein.
+*The E protein is necessary as a [[ligand]] to cell receptors and as a [[fusion protein]].
-*The other non-structural proteins serve as proteases, polymerases, complement binding antigens, or function within the replication process.
+*The other non-structural proteins serve as [[proteases]], [[polymerases]], complement binding [[antigens]], or function within the replication process.
-*Finally the processes concludes as the positive-stranded genome is translated while the negative-strand of RNA provides grounds for the RNA replication process.
+*Finally the processes concludes as the [[positive-stranded]] genome is translated while the negative-strand of RNA provides grounds for the RNA replication process.
-*Assembly of the virus occurs within the endoplasmic reticulum.
+*Assembly of the virus occurs within the [[endoplasmic reticulum]].
-*Post-assembly immature virions are released within the cell.<ref name="Enceph Prime">Tick-borne Encephalitis Virus: A General Overview. http://cdn.intechopen.com/pdfs-wm/20866.pdf. Accessed February 4, 2016. </ref>
+*Post-assembly immature [[virions]] are released within the cell.<ref name="Enceph Prime">Tick-borne Encephalitis Virus: A General Overview. http://cdn.intechopen.com/pdfs-wm/20866.pdf. Accessed February 4, 2016. </ref>
 ''Schematic drawing of the steps during TBE virus infection. (1) TBE virus transmission''
-from an infected tick, (2) TBE virus replication in regional lymph node, (3) primary viremia,
+from an infected tick, (2) TBE virus replication in regional lymph nodes, (3) primary viremia,
-(4) replication of the virus in other organs and tissues, (5) secondary viremia, (6) TBE virus
+(4) replication of the virus in other [[organs]] and [[Tissue (biology)|tissues]], (5) secondary viremia, (6) TBE virus
-crossing of the blood-brain barrier, and (7) virus infection of the brain''<ref name="Enceph Prime">Tick-borne Encephalitis Virus: A General Overview. http://cdn.intechopen.com/pdfs-wm/20866.pdf. Accessed February 4, 2016. </ref>]]''
+crossing of the [[blood-brain barrier]], and (7) virus infection of the brain''<ref name="Enceph Prime">Tick-borne Encephalitis Virus: A General Overview. http://cdn.intechopen.com/pdfs-wm/20866.pdf. Accessed February 4, 2016. </ref>]]''
 ===Viral pathway within a mammalian host===
-*Virus replication commonly occurs within subcutaneous tissue.
+*Virus replication commonly occurs within [[subcutaneous tissue]].
-*Dendritic cells transport the virus to the lymph nodes.
+*[[Dendritic cells]] transport the virus to the [[lymph nodes]].
-*The virus replicates at a high rate within the lymph nodes, further travelling into the bloodstream.
+*The virus replicates at a high rate within the [[lymph nodes]], further travelling into the bloodstream.
-*Lymphocytes suffer great reductions due to infection with the regional lymph nodes.
+*[[Lymphocytes]] suffer great reductions due to infection with the regional [[lymph nodes]].
-*Further infection of external tissues occur within the viremic phase
+*Further infection of external [[tissues]] occur within the [[Virus|viremic]] phase
 *The later phase results in the infection of the CNS.
-*Furthermore a host's immune system will add to the severity of the infection, as resulting immune response includes inflammation CD8+ T-cells infiltrating the brain.
+*Furthermore a host's [[immune system]] will add to the severity of the infection, as resulting immune response includes inflammation [[CD8+ T cells|CD8+ T-cells]] infiltrating the brain.
-*Other immune responses such as the upregulation of proinflammatory cytokines increase the permeability of the blood-brain barrier.<ref name="Enceph Prime">Tick-borne Encephalitis Virus: A General Overview. http://cdn.intechopen.com/pdfs-wm/20866.pdf. Accessed February 4, 2016. </ref>
+*Other immune responses such as the [[upregulation]] of [[proinflammatory]] [[Cytokine|cytokines]] increase the [[permeability]] of the [[blood-brain barrier]].<ref name="Enceph Prime">Tick-borne Encephalitis Virus: A General Overview. http://cdn.intechopen.com/pdfs-wm/20866.pdf. Accessed February 4, 2016. </ref>
 ==References==
 {{Reflist|2}}
 [[Category: Infectious Disease]]