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{{Main|Herpes simplex}}
{{Main|Herpes simplex}}


HSV-1 and -2 are transmitted from contact with an infectious area of the skin during reactivations of the virus. Although less likely, the herpes viruses can be transmitted during latency. Transmission is likely to occur during symptomatic reactivation of the virus that causes visible and typical skin sores. Asymptomatic reactivation means that the virus causes atypical, subtle or hard to notice symptoms that are not identified as an active herpes infection. Atypical symptoms are often attributed to other causes such as a yeast infection.<ref name="pmid18156035">{{cite journal |author=Gupta R, Warren T, Wald A |title=Genital herpes |journal=Lancet |volume=370 |issue=9605 |pages=2127–37 |year=2007 |pmid=18156035 |doi=10.1016/S0140-6736(07)61908-4}}</ref><ref name="PMID_18186706"/> HSV-1 is usually acquired orally during childhood, but may also be sexually transmitted. HSV-2 is primarily a sexually transmitted infection but rates of HSV-1 genital infections are increasing.<ref name="pmid18156035"/>
HSV-1 and -2 are transmitted from contact with an infectious area of the skin during reactivations of the virus. Although less likely, the herpes viruses can be transmitted during latency. Transmission is likely to occur during symptomatic reactivation of the virus that causes visible and typical skinS Esther Greene.=2780322}}</ref> The risk of infection is minimal if the mother has no symptoms or exposed blisters during delivery. The risk is considerable when the mother gets the virus for the first time during late pregnancy.<ref name="pmid17317423">{{cite journal |author=Kimberlin DW |title=Herpes simplex virus infections of the newborn |journal=Semin. Perinatol. |volume=31 |issue=1 |pages=19–25 |year=2007 |pmid=17317423 |doi=10.1053/j.semperi.2007.01.003}}</ref>

Both viruses may also be transmitted vertically during childbirth, although the real risk is very low.<ref name="pmid19797284">{{cite journal |author=Corey L, Wald A |title=Maternal and Neonatal Herpes Simplex Virus Infections |journal=New England Journal of Medicine |volume=361 |issue=14 |pages=1376–85 |year=2009 |pmid=19797284 |doi=10.1056/NEJMra0807633 |pmc=2780322}}</ref> The risk of infection is minimal if the mother has no symptoms or exposed blisters during delivery. The risk is considerable when the mother gets the virus for the first time during late pregnancy.<ref name="pmid17317423">{{cite journal |author=Kimberlin DW |title=Herpes simplex virus infections of the newborn |journal=Semin. Perinatol. |volume=31 |issue=1 |pages=19–25 |year=2007 |pmid=17317423 |doi=10.1053/j.semperi.2007.01.003}}</ref>


Symptoms resulting from primary infection with HSV are usually much more severe than subsequent outbreaks, as the body has not had a chance to produce [[antibodies]]. This first outbreak of oral herpes (cold sores) carries a low (≈1%) risk of developing [[aseptic meningitis]].<ref name=Sherris />
Symptoms resulting from primary infection with HSV are usually much more severe than subsequent outbreaks, as the body has not had a chance to produce [[antibodies]]. This first outbreak of oral herpes (cold sores) carries a low (≈1%) risk of developing [[aseptic meningitis]].<ref name=Sherris />

Revision as of 00:15, 4 October 2011

Herpes simplex virus
TEM micrograph of a herpes simplex virus.
Virus classification
Group:
Group I (dsDNA)
Family:
Subfamily:
Genus:
Species

Herpes simplex virus 1 (HSV-1)
Herpes simplex virus 2 (HSV-2)

Herpes simplex virus 1 and 2 (HSV-1 and HSV-2), also known as Human herpes virus 1 and 2 (HHV-1 and -2), are two members of the herpes virus family, Herpesviridae, that infect humans.[1] Both HSV-1 (which produces most cold sores) and HSV-2 (which produces most genital herpes) are ubiquitous and contagious. They can be spread when an infected person is producing and shedding the virus.

Symptoms of herpes simplex virus infection include watery blisters in the skin or mucous membranes of the mouth, lips or genitals.[1] Lesions heal with a scab characteristic of herpetic disease. Sometimes, the viruses cause very mild or atypical symptoms during outbreaks. However, as neurotropic and neuroinvasive viruses, HSV-1 and -2 persist in the body by becoming latent and hiding from the immune system in the cell bodies of nerves. After the initial or primary infection, some infected people experience sporadic episodes of viral reactivation or outbreaks. In an outbreak, the virus in a nerve cell becomes active and is transported via the nerve's axon to the skin, where virus replication and shedding occur and cause new sores.[2]

Transmission

HSV-1 and -2 are transmitted from contact with an infectious area of the skin during reactivations of the virus. Although less likely, the herpes viruses can be transmitted during latency. Transmission is likely to occur during symptomatic reactivation of the virus that causes visible and typical skinS Esther Greene.=2780322}}</ref> The risk of infection is minimal if the mother has no symptoms or exposed blisters during delivery. The risk is considerable when the mother gets the virus for the first time during late pregnancy.[3]

Symptoms resulting from primary infection with HSV are usually much more severe than subsequent outbreaks, as the body has not had a chance to produce antibodies. This first outbreak of oral herpes (cold sores) carries a low (≈1%) risk of developing aseptic meningitis.[1]

Microbiology

Viral structure

Animal herpes viruses all share some common properties. The structure of herpes viruses consists of a relatively large double-stranded, linear DNA genome encased within an icosahedral protein cage called the capsid, which is wrapped in a lipid bilayer called the envelope. The envelope is joined to the capsid by means of a tegument. This complete particle is known as the virion.[4] HSV-1 and HSV-2 each contain at least 74 genes (or open-reading frames, ORFs) within their genomes,[5] although speculation over gene crowding allows as many as 84 unique protein coding genes by 94 putative ORFs.[6] These genes encode a variety of proteins involved in forming the capsid, tegument and envelope of the virus, as well as controlling the replication and infectivity of the virus. These genes and their functions are summarized in the table below.

The genomes of HSV1 and HSV2 are complex and contain two unique regions called the long unique region (UL) and the short unique region (US). Of the 74 known ORFs, UL contains 56 viral genes, whereas US contains only 12.[5] Transcription of HSV genes is catalyzed by RNA polymerase II of the infected host.[5] Immediate early genes, which encode proteins that regulate the expression of early and late viral genes, are the first to be expressed following infection. Early gene expression follows, to allow the synthesis of enzymes involved in DNA replication and the production of certain envelope glycoproteins. Expression of late genes occurs last; this group of genes predominantly encode proteins that form the virion particle.[5]

Five proteins from (UL) form the viral capsid; UL6, UL18, UL35, UL38 and the major capsid protein UL19.[4]

Cellular entry

A simplified diagram of HSV replication

Entry of HSV into the host cell involves interactions of several glycoproteins on the surface of the enveloped virus, with receptors on the surface of the host cell. The envelope covering the virus particle, when bound to specific receptors on the cell surface, will fuse with the host cell membrane and create an opening, or pore, through which the virus enters the host cell.

The sequential stages of HSV entry are analogous to those of other viruses. At first, complementary receptors on the virus and the cell surface bring the viral and cell membranes into proximity. In an intermediate state, the two membranes begin to merge, forming a hemifusion state. Finally, a stable entry pore is formed through which the viral envelope contents are introduced to the host cell.[7] In the case of a herpes virus, initial interactions occur when a viral envelope glycoprotein called glycoprotein C (gC) binds to a cell surface particle called heparan sulfate. A second glycoprotein, glycoprotein D (gD), binds specifically to at least one of three known entry receptors. These include herpesvirus entry mediator(HVEM), nectin-1 and 3-O sulfated heparan sulfate. The receptor provides a strong, fixed attachment to the host cell. These interactions bring the membrane surfaces into mutual proximity and allow for other glycoproteins embedded in the viral envelope to interact with other cell surface molecules. Once bound to the HVEM, gD changes its conformation and interacts with viral glycoproteins H (gH) and L (gL), which form a complex. The interaction of these membrane proteins results in the hemifusion state. Afterward, gB interaction with the gH/gL complex creates an entry pore for the viral capsid.[7] Glycoprotein B interacts with glycosaminoglycans on the surface of the host cell.

Genetic inoculation

After the viral capsid enters the cellular cytoplasm, it is transported to the cell nucleus. Once attached to the nucleus at a nuclear entry pore, the capsid ejects its DNA contents via the capsid portal. The capsid portal is formed by twelve copies of portal protein, UL6, arranged as a ring; the proteins contain a leucine zipper sequence of amino acids which allow them to adhere to each other.[8] Each icosahedral capsid contains a single portal, located in one vertex.[9][10] The DNA exits the capsid in a single linear segment.[11]

Immune evasion

HSV evades the immune system through interference with MHC class I presentation of antigen on the cell surface. It achieves this through blockade of the TAP transporter induced by the secretion of ICP-47[12] by HSV. TAP maintains the integrity of the MHC class I molecule before it is transported via the golgi apparatus for recognition by CD8+ CTLs on the cell surface. ICP-47 disrupts this integrity, preventing the capture of cytosolic proteins for CTL recognition and thus evades CTL destruction.

Replication

Micrograph showing the viral cytopathic effect of HSV (multi-nucleation, ground glass chromatin).

Following infection of a cell, herpes virus proteins, called immediate-early, early, and late, are produced. Research using flow cytometry on another member of the herpes virus family, Kaposi's sarcoma-associated herpesvirus, indicates the possibility of an additional lytic stage, delayed-late.[13] These stages of lytic infection, particularly late lytic, are distinct from the latency stage. In the case of HSV-1, no protein products are detected during latency, whereas they are detected during the lytic cycle.

The early proteins transcribed are used in the regulation of genetic replication of the virus. On entering the cell, an α-TIF protein joins the viral particle and aids in immediate-early transcription. The virion host shutoff protein (VHS or UL41) is very important to viral replication.[14] This enzyme shuts off protein synthesis in the host, degrades host mRNA, helps in viral replication, and regulates gene expression of viral proteins. The viral genome immediately travels to the nucleus but the VHS protein remains in the cytoplasm.[15][16]

The late proteins are used in to form the capsid and the receptors on the surface of the virus. Packaging of the viral particles — including the genome, core and the capsid - occurs in the nucleus of the cell. Here, concatemers of the viral genome are separated by cleavage and are placed into pre-formed capsids. HSV-1 undergoes a process of primary and secondary envelopment. The primary envelope is acquired by budding into the inner nuclear membrane of the cell. This then fuses with the outer nuclear membrane releasing a naked capsid into the cytoplasm. The virus acquires its final envelope by budding into cytoplasmic vesicles.[17]

Latent infection

HSVs may persist in a quiescent but persistent form known as latent infection, notably in neural ganglia.[1] HSV-1 tends to reside in the trigeminal ganglia, while HSV-2 tends to reside in the sacral ganglia, but note that these are tendencies only, not fixed behavior. During such latent infection of a cell, HSVs express Latency Associated Transcript (LAT) RNA. LAT is known to regulate the host cell genome and interferes with natural cell death mechanisms. By maintaining the host cells, LAT expression preserves a reservoir of the virus, which allows subsequent, usually symptomatic, periodic recurrences or "outbreaks" characteristic of non-latency. Whether or not recurrences are noticeable (symptomatic) or not, viral shedding occurs to produce further infections (usually in a new host, if any). A protein found in neurons may bind to herpes virus DNA and regulate latency. Herpes virus DNA contains a gene for a protein called ICP4, which is an important transactivator of genes associated with lytic infection in HSV-1.[18] Elements surrounding the gene for ICP4 bind a protein known as the human neuronal protein Neuronal Restrictive Silencing Factor (NRSF) or human Repressor Element Silencing Transcription Factor (REST). When bound to the viral DNA elements, histone deacetylation occurs atop the ICP4 gene sequence to prevent initiation of transcription from this gene, thereby preventing transcription of other viral genes involved in the lytic cycle.[18][19] Another HSV protein reverses the inhibition of ICP4 protein synthesis. ICP0 dissociates NRSF from the ICP4 gene and thus prevents silencing of the viral DNA.[20]

The virus can be reactivated by illnesses such as colds and influenza, eczema, emotional and physical stress, gastric upset, fatigue or injury, by menstruation and possibly exposure to bright sunlight.

Viral genome

The open reading frames (ORFs) of HSV-1[5][21]
Gene Protein Function/description Gene Protein Function/description
UL1 Glycoprotein L [1] Surface and membrane UL38 UL38; VP19C [2] Capsid assembly and DNA maturation
UL2 UL2 [3] Uracil-DNA glycosylase UL39 UL39 [4] Ribonucleotide reductase (Large subunit)
UL3 UL3 [5] unknown UL40 UL40 [6] Ribonucleotide reductase (Small subunit)
UL4 UL4 [7] unknown UL41 UL41; VHS [8] Tegument protein; Virion host shutoff[14]
UL5 UL5 [9] DNA replication UL42 UL42 [10] DNA polymerase processivity factor
UL6 Portal protein UL-6 Twelve of these proteins constitute the capsid portal ring through which DNA enters and exits the capsid.[8][9][10] UL43 UL43 [11] Membrane protein
UL7 UL7 [12] Virion maturation UL44 Glycoprotein C [13] Surface and membrane
UL8 UL8 [14] DNA helicase/primase complex-associated protein UL45 UL45 [15] Membrane protein; C-type lectin[22]
UL9 UL9 [16] Replication origin-binding protein UL46 VP11/12 [17] Tegument proteins
UL10 Glycoprotein M [18] Surface and membrane UL47 UL47; VP13/14 [19] Tegument protein
UL11 UL11 [20] virion exit and secondary envelopment UL48 VP16 (Alpha-TIF) [21] Virion maturation; activate IEGs by interacting with the cellular transcription factors Oct-1 and HCF. Binds to the sequence 5'TAATGARAT3'.
UL12 UL12 [22] Alkaline exonuclease UL49 UL49A [23] Envelope protein
UL13 UL13 [24] Serine-threonine protein kinase UL50 UL50 [25] dUTP diphosphatase
UL14 UL14 [26] Tegument protein UL51 UL51 [27] Tegument protein
UL15 Terminase [28] Processing and packaging of DNA UL52 UL52 [29] DNA helicase/primase complex protein
UL16 UL16 [30] Tegument protein UL53 Glycoprotein K [31] Surface and membrane
UL17 UL17 [32] Processing and packaging DNA UL54 IE63; ICP27 [33] Transcriptional regulation
UL18 VP23 [34] Capsid protein UL55 UL55 [35] Unknown
UL19 VP5 [36] Major capsid protein UL56 UL56 [37] Unknown
UL20 UL20 [38] Membrane protein US1 ICP22; IE68 [39] Viral replication
UL21 UL21 [40] Tegument protein[23] US2 US2 [41] Unknown
UL22 Glycoprotein H [42] Surface and membrane US3 US3 [43] Serine/threonine-protein kinase
UL23 Thymidine kinase [44] Peripheral to DNA replication US4 Glycoprotein G [45] Surface and membrane
UL24 UL24 [46] unknown US5 Glycoprotein J [47] Surface and membrane
UL25 UL25 [48] Processing and packaging DNA US6 Glycoprotein D [49] Surface and membrane
UL26 P40; VP24; VP22A [50] Capsid protein US7 Glycoprotein I [51] Surface and membrane
UL27 Glycoprotein B [52] Surface and membrane US8 Glycoprotein E [53] Surface and membrane
UL28 ICP18.5 [54] Processing and packaging DNA US9 US9 [55] Tegument protein
UL29 UL29; ICP8 [56] Major DNA-binding protein US10 US10 [57] Capsid/Tegument protein
UL30 DNA polymerase [58] DNA replication US11 US11; Vmw21 [59] Binds DNA and RNA
UL31 UL31 [60] Nuclear matrix protein US12 ICP47; IE12 [61] Inhibits MHC class I pathway by preventing binding of antigen to TAP
UL32 UL32 [62] Envelope glycoprotein RS1 ICP4; IE175 [63] Major transcriptional activator. Essential for progression beyond the immediate-early phase of infection. IEG transcription repressor.
UL33 UL33 [64] Processing and packaging DNA ICP0 ICP0; IE110; α0 [65] E3 ubiquitin ligase that activates viral gene transcription and counteracts the interferon response
UL34 UL34 [66] Inner nuclear membrane protein LRP1 LRP1 [67] Latency-related protein
UL35 VP26 [68] Capsid protein LRP2 LRP2 [69] Latency-related protein
UL36 UL36 [70] Large tegument protein RL1 RL1; ICP34.5 [71] Neurovirulence factor. Antagonizes PKR by de-phosphorylating eIF4a.
UL37 UL37 [72] Capsid assembly LAT none [73] Latency-associated transcript

Treatment and vaccine development

For more details on treatment of herpes simplex virus, see Herpes simplex.
For more information on vaccines, see Herpes simplex vaccine

Herpes viruses establish lifelong infections and the virus cannot currently be eradicated from the body. Treatment usually involves general-purpose antiviral drugs that interfere with viral replication, reducing the physical severity of outbreak-associated lesions and lowering the chance of transmission to others. Studies of vulnerable patient populations have indicated that daily use of antivirals such as acyclovir and valacyclovir can reduce reactivation rates.[24]

In vitro research has indicated that Aloe Vera may be effective against genital herpes.[25]


Connection between facial sores and Alzheimer's disease

In the presence of a certain gene variation (APOE-epsilon4 allele carriers), a possible link between HSV-1 (i.e., the virus that causes cold sores or oral herpes) and Alzheimer’s disease was reported in 1979.[26] HSV-1 appears to be particularly damaging to the nervous system and increases one’s risk of developing Alzheimer’s disease. The virus interacts with the components and receptors of lipoproteins, which may lead to the development of Alzheimer's disease.[27] This research identifies HSVs as the pathogen most clearly linked to the establishment of Alzheimer’s.[28] Without the presence of the gene allele, HSV-1 does not appear to cause any neurological damage or increase the risk of Alzheimer’s.[29] Many more Alzheimer's disease susceptibility genes, including the major players APOE, clusterin, complement receptor 1 and PICALM are involved in the herpes simplex life cycle as curated in this database

References

  1. ^ a b c d Ryan KJ, Ray CG (editors) (2004). Sherris Medical Microbiology (4th ed.). McGraw Hill. pp. 555–62. ISBN 0838585299. {{cite book}}: |author= has generic name (help)
  2. ^ "Herpes simplex". DermNet NZ — New Zealand Dermatological Society. 2006-09-16. Retrieved 2006-10-15.
  3. ^ Kimberlin DW (2007). "Herpes simplex virus infections of the newborn". Semin. Perinatol. 31 (1): 19–25. doi:10.1053/j.semperi.2007.01.003. PMID 17317423.
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  6. ^ Rajcáni J, Andrea V, Ingeborg R (2004). "Peculiarities of herpes simplex virus (HSV) transcription: an overview". Virus Genes. 28 (3): 293–310. doi:10.1023/B:VIRU.0000025777.62826.92. PMID 15266111.{{cite journal}}: CS1 maint: multiple names: authors list (link)
  7. ^ a b Subramanian RP, Geraghty RJ (2007). "Herpes simplex virus type 1 mediates fusion through a hemifusion intermediate by sequential activity of glycoproteins D, H, L, and B". Proc. Natl. Acad. Sci. U.S.A. 104 (8): 2903–8. doi:10.1073/pnas.0608374104. PMC 1815279. PMID 17299053.
  8. ^ a b Cardone G, Winkler DC, Trus BL, Cheng N, Heuser JE, Newcomb WW, Brown JC, Steven AC (2007). "Visualization of the herpes simplex virus portal in situ by cryo-electron tomography". Virology. 361 (2): 426–34. doi:10.1016/j.virol.2006.10.047. PMC 1930166. PMID 17188319. {{cite journal}}: Unknown parameter |month= ignored (help)CS1 maint: multiple names: authors list (link) Cite error: The named reference "pmid17188319" was defined multiple times with different content (see the help page).
  9. ^ a b Trus BL, Cheng N, Newcomb WW, Homa FL, Brown JC, Steven AC (2004). "Structure and polymorphism of the UL6 portal protein of herpes simplex virus type 1". Journal of Virology. 78 (22): 12668–71. doi:10.1128/JVI.78.22.12668-12671.2004. PMC 525097. PMID 15507654. {{cite journal}}: Unknown parameter |month= ignored (help)CS1 maint: multiple names: authors list (link)
  10. ^ a b Nellissery JK, Szczepaniak R, Lamberti C, Weller SK (2007-06-20). "A putative leucine zipper within the HSV-1 UL6 protein is required for portal ring formation". Journal Virology. 81 (17): 8868–77. doi:10.1128/JVI.00739-07. PMC 1951442. PMID 17581990.{{cite journal}}: CS1 maint: multiple names: authors list (link)
  11. ^ Newcomb WW, Booy FP, Brown JC (2007). "Uncoating the herpes simplex virus genome". J. Mol. Biol. 370 (4): 633–42. doi:10.1016/j.jmb.2007.05.023. PMC 1975772. PMID 17540405.{{cite journal}}: CS1 maint: multiple names: authors list (link)
  12. ^ Abbas et al (2009) Cellular and Molecular Immunology, Elsevier Inc.
  13. ^ Adang LA, Parsons CH, Kedes DH (2006). "Asynchronous progression through the lytic cascade and variations in intracellular viral loads revealed by high-throughput single-cell analysis of Kaposi's sarcoma-associated herpesvirus infection". J. Virol. 80 (20): 10073–82. doi:10.1128/JVI.01156-06. PMC 1617294. PMID 17005685.{{cite journal}}: CS1 maint: multiple names: authors list (link)
  14. ^ a b Matis J, Kúdelová M (2001). "Early shutoff of host protein synthesis in cells infected with herpes simplex viruses". Acta Virol. 45 (5–6): 269–77. PMID 12083325.
  15. ^ Taddeo B, Roizman B (2006). "The virion host shutoff protein (UL41) of herpes simplex virus 1 is an endoribonuclease with a substrate specificity similar to that of RNase A". J. Virol. 80 (18): 9341–5. doi:10.1128/JVI.01008-06. PMC 1563938. PMID 16940547.
  16. ^ Skepper JN, Whiteley A, Browne H, Minson A (2001). "Herpes simplex virus nucleocapsids mature to progeny virions by an envelopment --> deenvelopment --> reenvelopment pathway". J. Virol. 75 (12): 5697–702. doi:10.1128/JVI.75.12.5697-5702.2001. PMC 114284. PMID 11356979. {{cite journal}}: Unknown parameter |month= ignored (help)CS1 maint: multiple names: authors list (link)
  17. ^ Granzow H, Klupp BG, Fuchs W, Veits J, Osterrieder N, Mettenleiter TC (2001). "Egress of alphaherpesviruses: comparative ultrastructural study". J. Virol. 75 (8): 3675–84. doi:10.1128/JVI.75.8.3675-3684.2001. PMC 114859. PMID 11264357. {{cite journal}}: Unknown parameter |month= ignored (help)CS1 maint: multiple names: authors list (link)
  18. ^ a b Pinnoji RC, Bedadala GR, George B, Holland TC, Hill JM, Hsia SC (2007). "Repressor element-1 silencing transcription factor/neuronal restrictive silencer factor (REST/NRSF) can regulate HSV-1 immediate-early transcription via histone modification". Virol. J. 4: 56. doi:10.1186/1743-422X-4-56. PMC 1906746. PMID 17555596.{{cite journal}}: CS1 maint: multiple names: authors list (link) CS1 maint: unflagged free DOI (link)
  19. ^ Bedadala GR, Pinnoji RC, Hsia SC (2007). "Early growth response gene 1 (Egr-1) regulates HSV-1 ICP4 and ICP22 gene expression". Cell Res. 17 (6): 546–55. doi:10.1038/cr.2007.44. PMID 17502875.{{cite journal}}: CS1 maint: multiple names: authors list (link)
  20. ^ Roizman B, Gu H, Mandel G (2005). "The first 30 minutes in the life of a virus: unREST in the nucleus". Cell Cycle. 4 (8): 1019–21. PMID 16082207.{{cite journal}}: CS1 maint: multiple names: authors list (link)
  21. ^ Search in UniProt Knowledgebase (Swiss-Prot and TrEMBL) for: HHV1
  22. ^ Wyrwicz LS, Ginalski K, Rychlewski L (2007). "HSV-1 UL45 encodes a carbohydrate binding C-type lectin protein". Cell Cycle. 7 (2): 269–71. doi:10.4161/cc.7.2.5324. PMID 18256535.{{cite journal}}: CS1 maint: multiple names: authors list (link)
  23. ^ Vittone V, Diefenbach E, Triffett D, Douglas MW, Cunningham AL, Diefenbach RJ (2005). "Determination of interactions between tegument proteins of herpes simplex virus type 1". J. Virol. 79 (15): 9566–71. doi:10.1128/JVI.79.15.9566-9571.2005. PMC 1181608. PMID 16014918.{{cite journal}}: CS1 maint: multiple names: authors list (link)
  24. ^ Koelle DM, Corey L (2008). "Herpes simplex: insights on pathogenesis and possible vaccines". Annual Review of Medicine. 59: 381–95. doi:10.1146/annurev.med.59.061606.095540. PMID 18186706.
  25. ^ Vogler BK, Ernst E (1999). "Aloe vera: a systematic review of its clinical effectiveness". The British Journal of General Practice. 49 (447): 823–8. PMC 1313538. PMID 10885091. {{cite journal}}: Unknown parameter |month= ignored (help)
  26. ^ Middleton PJ, Petric M, Kozak M, Rewcastle NB, McLachlan DR (1980). "Herpes-simplex viral genome and senile and presenile dementias of Alzheimer and Pick". Lancet. 315 (8176): 1038. doi:10.1016/S0140-6736(80)91490-7. PMID 6103379. {{cite journal}}: Unknown parameter |month= ignored (help)CS1 maint: multiple names: authors list (link)
  27. ^ Dobson CB, Itzhaki RF (1999). "Herpes simplex virus type 1 and Alzheimer's disease". Neurobiol. Aging. 20 (4): 457–65. doi:10.1016/S0197-4580(99)00055-X. PMID 10604441.
  28. ^ Pyles RB (2001). "The association of herpes simplex virus and Alzheimer's disease: a potential synthesis of genetic and environmental factors" (PDF). Herpes. 8 (3): 64–8. PMID 11867022. {{cite journal}}: Unknown parameter |month= ignored (help)
  29. ^ Itzhaki RF, Lin WR, Shang D, Wilcock GK, Faragher B, Jamieson GA (1997). "Herpes simplex virus type 1 in brain and risk of Alzheimer's disease". Lancet. 349 (9047): 241–4. doi:10.1016/S0140-6736(96)10149-5. PMID 9014911. {{cite journal}}: Unknown parameter |month= ignored (help)CS1 maint: multiple names: authors list (link)