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H. P. Ossent 《TAG. Theoretical and applied genetics. Theoretische und angewandte Genetik》1930,2(8):221-227
Ohne Zusammenfassung 相似文献
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H. P. Ossent 《TAG. Theoretical and applied genetics. Theoretische und angewandte Genetik》1932,4(9):230-231
Ohne ZusammenfassungVorläufige Mitteilung. 相似文献
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Husfeld H. v. Rathlef v. Rauch P. Hertwig Hackbarth Oehler v. Berg Schmidt Michaelis Stubbe Hackbarth W. von Wettstein-Westersheim Hackbarth Rudorf Ossent H. v. Rathlef v. Rosenstiel Kuckuck Ufer F. Gruber 《TAG. Theoretical and applied genetics. Theoretische und angewandte Genetik》1935,7(2):48-56
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The objective of this study was to find a reliable alternative to Freund's adjuvant in order to reduce the distress imposed on the animals without impairing the fusion efficiency for immune-positive clones. For this purpose several commercially available adjuvants and adjuvant formulations representing different classes of molecules were compared. Humoral responses and animals' distress evaluated by clinical assessment and histopathological examinations were investigated and compared to fusion efficiencies. In a first set of experiments seven adjuvants were tested essentially to determine their potential to induce distress. Poly(A).poly(U) and GERBU were selected for further investigations due to their low overall toxicity. They were combined with five different antigens and compared to the classic Freund's adjuvant system (CFA/IFA) and to control immunizations without adjuvant. The results showed that adjuvants of very low toxicity could induce a high fusion efficiency. According to a standardized immunization protocol, GERBU induced polyclonal titres similar to Freund's whereas animals treated with poly(A).poly(U) did not attain titres higher than mice immunized with antigen in saline. Poly(A).poly(U) however, exhibited the best fusion efficiency, Freund and GERBU were slightly less efficient. Therefore poly(A).poly(U) and GERBU may serve as valuable alternatives to Freund's adjuvant for generating monoclonal antibodies. Furthermore, these two adjuvants are very easy to use. 相似文献
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BACKGROUND AND PURPOSE: The existence of guinea pig adenovirus (GPAdV) has been suspected on the basis of histopathologic findings, but the virus has not yet been isolated. In susceptible animals, it may cause severe bronchopneumonia and death. Adenovirus-like inclusion bodies have been observed in the lungs of animals with clinical disease. Prevalence of the infection is unknown. Recently, a polymerase chain reaction (PCR) assay was described that was able to selectively detect GPAdV. METHODS: To investigate the pathogenesis of GPAdV, we inoculated eight guinea pigs with GPAdV; eight control animals were sham inoculated. The PCR assay was used to trace the infection. In a second experiment, transmission of GPAdV from an experimentally infected animal to five immune-naive cohorts was examined. RESULTS: None of the infected animals developed clinical disease. The GPAdV could be detected by PCR analysis of nasal-swab specimens on days 6 through 15 after infection. Infective virus could be recovered from the nasal mucosa during this period (as determined by inoculation of immune-naive animals). The virus was transmitted from an experimentally infected animal to two of five immune-naive cage mates. CONCLUSION: The GPAdV may cause transient subclinical upper respiratory tract infection that may descend to the lungs. 相似文献
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H. P. Ossent 《TAG. Theoretical and applied genetics. Theoretische und angewandte Genetik》1929,1(1):11-13
Ohne ZusammenfassungMit 6 Abbildungen. 相似文献