Specific restriction in the progression of Venezuelan equine encephalitis virus-induced disease resulting from single amino acid changes in the glycoproteins.

Grieder F.B.; Davis N.L.; Aronson J.F.; Charles P.C.; Sellon D.C.; Suzuki K.; Johnson R.E.

Specific restriction in the progression of Venezuelan equine encephalitis virus-induced disease resulting from single amino acid changes in the glycoproteins.

1995

The pathogenesis of Venezuelan equine encephalitis virus (VEE) was examined in the mouse model using V3000, a virus derived from a molecular clone of the Trinidad donkey strain of VEE. These results were compared in parallel experiments with avirulent mutants of VEE derived by site-directed mutagenesis of the clone. Adult mice, inoculated subcutaneously in their left rear footpad with V3000, were followed in a time course study for 6 days in which 15 organs were tested for histopathological changes, for the presence of viral antigen by immunohistochemical staining, for the presence of viral nucleic acid by in situ hybridization analysis, and for content of viable virus. Virus was detected in the footpad inoculation site, but until 12 hr postinoculation (pi), the level of virus did not suggest early viral replication. By 4 hr pi, however, replication of V3000 was evident in the draining popliteal lymph node. At this early time point, no virus could be isolated from any other organ examined. At 12 hr, a significant serum viremia was observed, and virus was detected at a low level in a number of well vascularized organs, including spleen, heart, lung, liver, kidney, and adrenal gland. By 18 hr, high virus titers were present in serum and all the lymphoid organs examined, and these tissues appeared to be the major peripheral sites of V3000 replication. Virus in serum and peripheral organs was cleared by 3-4 days pi. In a second phase of the infection, V3000 invaded the central nervous system (CNS), replicated predominantly in neurons, and persisted in the brain until death by encephalitis. Pathologic findings as well as the results of immunocytochemical and in situ hybridization examination were generally coordinate with virus titration. A site-directed mutant of V3000, V3010, contained a mutation in the gene for the E2 glycoprotein at codon 76 (Glu to Lys) which rendered it avirulent after footpad inoculation.

اظهر المزيد [+]

الكلمات المفتاحية الخاصة بالمكنز الزراعي (أجروفوك)

alphavirus antigene antigens chemistry chimie clone clones glycoproteins histopathologie histopathology histopatologia immunologie immunology mice mutant mutantes mutants mutation pathogenicity souris

المعلومات البيبليوغرافية

نُشرت في

Virology

المجلد 206 الرقم التسلسلي المعياري الدولي (ردمد) 0042-6822

ترقيم الصفحات

v.994-1006(2)

مواضيع أخرى

Quimica; Poder patogeno; Glycoproteine; Raton; Mutacion; Inmunologia; Antigenos; Glicoproteinas; Pouvoir pathogene

اللغة

إنجليزي

ملاحظة

references. AVAILABILITY: US (DNAL 448.8 V81).

النوع

Journal Article; Journal Part

المصدر

Virology (USA). (1 Feb 1995). v. 206(2) p. 994-1006.

مؤسسة مؤلف

Uniformed Services University of the Health Sciences, Bethesda, MD.

في أجريس منذ: 2012-11-15

نوع الملف: AGRIS AP

مزود البيانات

تم تزويد هذا السجل من قبل Wolters Kluwer

اكتشف مجموعة مزود البيانات هذا في أجريس

تصفح الباحث العلمي من جوجل

إذا لاحظت أي معلومات غير صحيحة تتعلق بهذا السجل ، يرجى الاتصال بنا [email protected]

أجريس - النظام الدولي للعلوم الزراعية والتكنولوجيا

Share

Specific restriction in the progression of Venezuelan equine encephalitis virus-induced disease resulting from single amino acid changes in the glycoproteins.

1995

الكلمات المفتاحية الخاصة بالمكنز الزراعي (أجروفوك)

المعلومات البيبليوغرافية