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1. |
Ocular pathogenicity of herpes simplex virus |
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Current Eye Research,
Volume 6,
Issue 1,
1987,
Page 1-7
HillTerry J.,
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摘要:
As a relatively small, discrete organ that contains a number of widely different cell types the eye provides an intriguing system in which to study fundamental aspects of virus/cell interactions. Such aspects are considered with particular reference to herpes simplex virus and the pivotal role of virus/neuron interactions in the development of ocular disease. Three aspects of this interaction are discussed: i) the entry of virus into the eye ii) latency in the trigeminal ganglion iii) nerve damage.
ISSN:0271-3683
DOI:10.3109/02713688709020060
出版商:Taylor&Francis
年代:1987
数据来源: Taylor
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2. |
Spread of HSV-1 to the mouse eye after inoculation in the skin of the snout requires an intact nerve supply to the inoculation site |
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Current Eye Research,
Volume 6,
Issue 1,
1987,
Page 9-12
ShimeldC.,
DysonH.,
LewkowiczS.,
HillT. J.,
BlythW. A.,
EastyD. L.,
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摘要:
Infection of the eye following inoculation of herpes simplex virus on the skin of the snout was monitored using slit lamp examination of the eye, isolation of virus from eyewashings and identification of virus antigens in whole corneal epithelial sheets by peroxidase-antiperoxidase staining. Infection of the eye was prevented by removing a section of the sensory nerves which supply the inoculation site. This provided evidence that spread from the skin of the snout to the eye occurred via the nerves.
ISSN:0271-3683
DOI:10.3109/02713688709020061
出版商:Taylor&Francis
年代:1987
数据来源: Taylor
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3. |
Adenosine deaminase in herpes simplex virus induced corneal stromal disease |
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Current Eye Research,
Volume 6,
Issue 1,
1987,
Page 13-18
O'brienWilliam J.,
TaylorJerry L.,
BrotmanSteven J.,
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摘要:
The development of herpes simplex virus (HSV)-induced disciform stromal disease produced by the intrastromal injection of the RE strain of HSV-1 is characterized by concurrent increases in adenosine deaminase (ADA) activity and corneal thickness. ADA activity increased from 8.6 units/cornea in normal corneas to about 14.1 units and 31.1 units in mock-infected controls and HSV-infected corneas respectively by 15 days postinjection. The molecular weight species of ADA in the corneas of HSV-infected rabbits appeared altered relative to that present in corneas which were not infected. A single topical dose with as low as 0.1% 2-deoxycoformycin (dCF), an ADA inhibitor possessing immunosuppressive activity, was capable of totally inhibiting the corneal ADA activity. Titration of the free dCF in the cornea following a single topical dose of 0.25% dCF indicated that enough dCF remained in the cornea 24 hrs after instillation to totally inhibit all corneal ADA plus 66 units of additional enzyme. These data suggest that ADA may be a suitable target for immunosuppressive therapy during HSV-induced disciform stromal disease.
ISSN:0271-3683
DOI:10.3109/02713688709020062
出版商:Taylor&Francis
年代:1987
数据来源: Taylor
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4. |
Nucleotide sequences important in DNA replication are responsible for differences in the capacity of two herpes simplex virus strains to spread from cornea to central nervous system |
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Current Eye Research,
Volume 6,
Issue 1,
1987,
Page 19-26
DayS. P.,
LauschR. N.,
OakesJ. E.,
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摘要:
Two herpes simplex virus (HSV) intertypic recombinants were isolated with genomes composed entirely of HSV-2(186) nucleotide sequences except for a 6.0 Kb segment of HSV-1(17) DNA positioned between 0.40 and 0.44 map units. Following corneal infection of mice, HSV-1(17) and the two intertypic recombinants spread from infected eyes into the central nervous system and induced a fatal encephalitis. Ocular infection with the HSV-2 (186) parent did not lead to detectable amounts of virus in the brain, and none of the mice developed encephalitis. The 6.0 Kb HSV-1(17) DNA inserted within the genome of the two intertypic recombinants contained nucleotide sequences involved in DNA replication. These include the HSV-1(17)oriL, the HSV-1(17) gene for DNA polymerase and portions of the HSV-1(17) gene coding for DNA-binding protein ICP8. Thus, our results indicate that the difference in the capacity of HSV-1(17) and HSV-2(186) to spread from the cornea into the CNS is determined solely by nucleotide sequences associated with DNA replication.
ISSN:0271-3683
DOI:10.3109/02713688709020063
出版商:Taylor&Francis
年代:1987
数据来源: Taylor
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5. |
Failure of intertypic recombinant constructed from HSV-1×HSV-2 virulent parents to induce ocular pathology |
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Current Eye Research,
Volume 6,
Issue 1,
1987,
Page 27-32
LauschRobert N.,
LeeJ. Dennis,
OakesJohn E.,
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摘要:
An intertypic recombinant constructed from HSV-1×HSV-2 parents was isolated which failed to induce any overt ocular pathology when inoculated onto the sacrificed cornea of four-week-old SJL/J mice. During the 24-48 hour post-infection period there was transient virus replication but by day 3 the infectious titer in the eye had dropped by≥104-fold, and little or no virus could be recovered thereafter. When immunosuppressed (600 r) mice were infected corneally, virus clearance was delayed several days but again no obvious ocular pathology was seen, and no mice died. By contrast, infection of the cornea with either parent was followed by virus replication and development of clinically apparent pathology which could progress to blinding stromal keratitis. The genome of the intertypic recombinant was analyzed by agarose gel electrophoresis of restriction endonuclease digests and found to consist entirely of HSV-1 DNA except for HSV-2 DNA sequences located between map units 0.10–0.16, 0.41–0.43, and 0.77–1.0. Potential explanations for the loss of virulence are discussed.
ISSN:0271-3683
DOI:10.3109/02713688709020064
出版商:Taylor&Francis
年代:1987
数据来源: Taylor
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6. |
Analysis of glycoproteins expressed by isolates of herpes simplex virus causing different forms of keratitis in man |
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Current Eye Research,
Volume 6,
Issue 1,
1987,
Page 33-38
TulloA. B.,
CoupesD.,
KlapperP.,
CleatorG.,
ChitkaraD.,
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摘要:
Anin vitroanalysis of glycoprotein produced by nine human ocular isolates of HSV-1 is reported. The source of the isolates was; three patients with recurrent dendritic keratitis, three with chronic stromal disease and three with primary keratoconjunctivitis. Virus strains were labelled with the radioactive precursors (35s) methionine and (14c) glucosamine. Radiolabelled viral glycoproteins were subsequently analysed by sodium dodecyl sulphate polyacrylamide gel electrophoresis (SDS-PAGE), followed by autoradiography. Viral glycoproteins were further characterised by immuno-precipitation with polyclonal and monoclonal antibodies to HSV. The stromal isolates excrete larger amounts of 'soluble' precursor glycoprotein D than those in the other two disease categories. It is possible that the immune response to glycoprotein D is in part responsible for the severity of stromal disease.
ISSN:0271-3683
DOI:10.3109/02713688709020065
出版商:Taylor&Francis
年代:1987
数据来源: Taylor
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7. |
HSV1 strain sensitivity in experimental rabbit keratitis: evolution under repeated topical IDU administrations |
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Current Eye Research,
Volume 6,
Issue 1,
1987,
Page 39-45
DenisJ.,
LangloisM.,
ElkaimM.,
AmielC.,
AymardM.,
HurauxJ. M.,
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摘要:
The effects of repeated topical idoxuridine (IDU) administration on HSV1 strain sensitivity were investigated during 6 serial passages (P1 to P6) in the rabbit. By comparison to placebo treated rabbits, a delay in ulcer cicatrization appeared at P2 and clinical resistance was completed at P3. Clinical cross resistance to acyclovir (ACV) was also tested and demonstrated at P7. In vitro, a plaque reduction test on Vero cells using directly the tear film HSV populations allowed the prediction of the resistance by an early rise in the effective dose 90 % (ED 90) value anticipating that in ED 50 %. An ED 50 determination by dye-uptake assay on P6 HSV isolate demonstrated a cross resistance to viral thymidine kinase (TK) dependent drugs without any change in Ara-A and PFA sensitivity, according to a 23 % TK activity at P6. At the last passage the HSV drug resistant population had an unrestricted corneal pathogenicity. A return to IDU and ACV in vitro sensitivity was demonstrated in group control animals at P2 but not at P4 or P6.
ISSN:0271-3683
DOI:10.3109/02713688709020066
出版商:Taylor&Francis
年代:1987
数据来源: Taylor
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8. |
Histopathologic characteristics of two forms of experimental herpes simplex virus retinitis |
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Current Eye Research,
Volume 6,
Issue 1,
1987,
Page 47-52
DixRichard D.,
StreileinJ. Wayne,
CousinsScott,
AthertonSally S.,
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摘要:
Herpes simplex virus type 1 (HSV-1) inoculated intracamerally into one anterior chamber of a BALB/c mouse produces retinitis in the uninoculated contralateral eye within 7 to 10 days while the retina of the inoculated eye is spared. In sharp contrast, animals receiving HSV type 2 (HSV-2) by the anterior chamber route develop a dramatic retinitis in theinoculatedeye by day 7 postinoculation while the retina of the contralateral eye remains uninvolved. Histopathologic examination of retinal destruction in the HSV-2-infected ipsilateral eye revealed features which were distinct from those observed in the contralateral eye of HSV-1-infected animals. Whereas HSV-1 produced a rapid, explosive, retinitis which led to destruction of all cell layers of the contralateral retina, HSV-2 induced a retinitis in the ipsilateral eye that was more gradual in onset. Ipsilateral HSV-2 retinitis was characterized initially by disruption of the ganglion and inner nuclear layers which progressed by day 10 to 14 to complete replacement of the retina by a fibrocellular scar. These changes were dominated by a vigorous mononuclear cell infiltrate, a feature not observed in the HSV-1-infected contralateral retinitis. These results suggest that experimental retinitides produced by HSV-1 and HSV-2 are of diverse pathogenesis.
ISSN:0271-3683
DOI:10.3109/02713688709020067
出版商:Taylor&Francis
年代:1987
数据来源: Taylor
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9. |
Effect of neuraminidase on Fc and C3b receptors on rabbit corneal cells infected with herpes simplex virus |
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Current Eye Research,
Volume 6,
Issue 1,
1987,
Page 53-58
HatanoHiroshi,
OhJang O.,
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摘要:
The effect of neuraminidase on Fc receptors (FcR) and C3b receptors (C3bR) was studied in epithelial, stromal and endothelial cells of the rabbit cornea infected with type 1 (HSV-1) and type 2 herpes simplex virus (HSV-2)in vitro. FcR were induced on epithelial, stromal and endothelial cells of the rabbit cornea by both HSV-1 and HSV-2, but their activities were not enhanced by neuraminidase. On the other hand, the treatment of HSV-infected corneal cells with neuraminidase resulted in the enhancement of C3bR activities on epithelial, stromal and endothelial cells infected with HSV-1, and the enhancing effect of neuraminidase was more pronounced on corneal endothelial cells. A similar neuraminidase treatment had no significant effect on C3bR activities on the corneal cells infected with HSV-2.
ISSN:0271-3683
DOI:10.3109/02713688709020068
出版商:Taylor&Francis
年代:1987
数据来源: Taylor
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10. |
Routes of viral spread in the von Szily model of herpes simplex virus retinopathy |
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Current Eye Research,
Volume 6,
Issue 1,
1987,
Page 59-62
OlsonRobert M.,
HollandGary N.,
GossSusan J.,
BowersWynnwood D.,
MeyersRoberta H.,
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摘要:
Intraocular inoculation of herpes simplex virus type 1 (HSV-1) in one eye of rabbits results in encephalitis and contralateral necrotizing viral retinopathy. The effects of viral inoculation site and optic nerve (ON) transection on the spread of virus to the brain and contralateral eye in this model were investigated. A surgical technique was developed for transection of the retrobulbar optic nerve posterior to the entrance of the central retinal vessels. HSV-1 was inoculated into the AC or vitreous of one eye in normal rabbits and in rabbits with one ON transected, either ipsilateral or contralateral to the side of inoculation. Animals were followed clinically for signs of disease. Encephalitis and contralateral retinopathy (CR) occurred following both AC and vitreous inoculation of virus, although CR developed later in AC-inoculated rabbits. Ipsilateral retinopathy (IR) developed in 83% of vitreous-inoculated rabbits, but in only 5% of AC-inoculated animals. IR developed 8 days after the onset of CR in the AC-inoculated group. ON transection on the side of virus inoculation prevented development of CR only in vitreous-inoculated rabbits. ON transection on the side opposite virus inoculation prevented CR regardless of the site of inoculation. These findings suggest that HSV-1 can leave the inoculated eye by multiple routes depending on the site of virus inoculation, but that virus reaches the retina of the contralateral eye via the optic nerve.
ISSN:0271-3683
DOI:10.3109/02713688709020069
出版商:Taylor&Francis
年代:1987
数据来源: Taylor
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