Translation of "Semliki forest virus" in German

Particularly preferred viruses which may be used in the practice of the invention include Adenovirus subgroup C, type 5, Semliki Forest Virus, Vesicular Stomatitis Virus, Poliovirus, Rhinoviruses and Moloney Leukemia Virus.

In a preferred embodiment, a fusion protein (c) is selected from the group consisting of hemagglutinin or influenza A or B viruses, the HA2 component of the hemagglutinin or influenza A or B viruses and peptide analogs thereof, the M2 protein of influenza A viruses, the HEF protein of influenza C viruses, a transmembrane protein of filoviruses such as Marburg virus or Ebola virus, a transmembrane glycoprotein of rabies virus, vesicular stomatitis virus, Semliki Forest virus, tickborn encephalitis virus, a fusion protein of HIV virus, Sendai virus (in particular the F1 component) or respiratory syncytial virus (in particular the gp37 component) and fragments of these viral fusion proteins or of the transmembrane glycoproteins that contain the fusiogenic peptides.

The vector as claimed in claim 1, wherein said fusion protein (c) is selected from the group consisting of hemagglutinin of influenza A or B viruses, the HA2 component of the hemagglutinin of influenza A or B viruses, a peptide analogue thereof, the M2 protein of influenza A viruses, the HEF protein of influenza C viruses, a transmembrane protein of filoviruses, a transmembrane glycoprotein of rabies virus, vesicular stomatitis virus, Semliki Forest virus, tickborn encephalitis virus, a fusion protein of HIV virus, Sendai virus, respiratory syncytial virus, and a fragment of said viral fusion proteins or of transmembrane glycoprotein from said viruses from which the transmembrane region is removed.

In a preferred embodiment, a viral vector for administering a nucleic acid coding for a tumor-associated antigen is selected from the group consisting of adenoviruses, adeno-associated viruses, pox viruses, including vaccinia virus and attenuated pox viruses, Semliki Forest virus, retroviruses, Sindbis virus and Ty virus-like particles.

We express the GPCRs and their interaction partners in Pichia pastoris, in insect cells, and in mammalian cells using the Semliki Forest Virus expression system.

In a preferred embodiment, a viral vector for administering a nucleic acid which codes for a fusion molecule of the invention is selected from the group consisting of adenoviruses, adeno-associated viruses, poxviruses, including vacciniavirus and attenuated poxviruses, Semliki forest virus, retroviruses, Sindbis virus and Ty virus-like particles.

The transient expression in mammalian cell lines is generally based on the transfection of a plasmid vector incorporating the expression cassette with the sequence encoding the desired gene product. Also viral expression vectors such as Semliki Forest virus or adenovirus can be used but they are uncommon since they are efficient but time-consuming and connected with high safety requirements.

Alternatively, several other viruses are also qualified e.g. recombinant alpha-viruses, e.g. the Semliki-Forest virus or the Venezuela-Enzphalitis virus, recombinant adenoviruses, recombinant Herpes simplex viruses, influenza viruses and others.

The C 15 alkyl monoesters of general formula I were also capable of inactivating the Semliki-Forest virus (SFV) within 20 minutes at a concentration of 40 ?M by a factor of >10 4 .

Predominantly, viruses which can be inactivated by means of the method of the invention are herpes viruses preferably HSV-1, HSV-2, BHV-1, SHV-1, immunodeficiency viruses, preferably HIV-1, HIV-2, SIV agm, the vesicular stomatitis virus (VSV), and the Semliki-Forest virus (SFV).