| 发明名称 |
Method for identifying t-cell stimulating protein fragments |
| 摘要 |
The invention relates to a method for identifying T-cell stimulating protein fragments using the following steps: a) detecting the amino acid sequence of an antigen; b) subdividing the found amino acid sequence of the antigen into protein fragments; c) synthesizing at least one protein fragment; d) incubating a suspension containing t-cells with the protein fragments; e) identifying an induced T-cell cytokine or activation marker by flow-through cytometry, and; f) assigning the T-cells, with which T-cell cytokines and/or activation markers were identified, to the protein fragments which were incubated with the T-cells. The corresponding protein fragments/peptides are synthetically produced with the assistance of the detected positive sequence, and said corresponding protein fragments/peptides can be utilized to produce a medicament for immunostimulation. |
| 申请公布号 |
US8932806(B1) |
申请公布日期 |
2015.01.13 |
| 申请号 |
US199909600564 |
申请日期 |
1999.01.15 |
| 申请人 |
|
发明人 |
Kern Florian;Volk Hans-Dieter;Walden Peter;Scheffold Alexander;Blasczyk Rainer |
| 分类号 |
C12Q1/00;A61K45/00;A01N63/00 |
主分类号 |
C12Q1/00 |
| 代理机构 |
Norris McLaughlin & Marcus, P.A. |
代理人 |
Norris McLaughlin & Marcus, P.A. |
| 主权项 |
1. A method for the identification of T-cell stimulating protein fragments comprising the following steps:
a) establishing the amino acid sequence of an antigen which is a protein or a peptide; b) synthesizing at least one protein fragment having a length of from 8 to 30 amino acids, or cleaving said antigen to yield at least one protein fragment having a length of from 8 to 30 amino acids, wherein said protein fragment has an amino acid sequence which is a subsequence of the established amino acid sequence of said antigen; c) incubating a suspension containing T cells with the protein fragment or fragments in different experimental runs for an incubation time, the incubation time being sufficiently long that the protein fragment or fragments are sufficiently taken up by the major histocompatibility antigen (MHC) molecules present on the cellular surface, said protein fragment or fragments being sufficiently taken up by the MHC molecules when an unambiguous identification of stimulated T cells is possible, and the incubation time being sufficiently short that selection and proliferation of stimulated T-cells do not occur; d) identifying
(i) at least one T cell cytokine which has been induced by the protein fragment or fragments and synthesized in the T cells, wherein the T cell cytokine or cytokines remain within the cell or are bound to the cell membrane; and/or(ii) at least one activation marker is expressed or the expression of the marker is increased due to the T cell stimulation by the protein fragment or fragments wherein said activation marker can be present within the cell or expressed on the cellular surface;wherein said T cell cytokine or cytokines or activation markers are identified by flow cytometry; and
e) assigning the experimental runs in which T cells have been stimulated and such stimulation has been recognized by the identification of one or more T cell cytokines and/or one or more activation markers, to the amino acid sequence or sequences of said protein fragments which had been incubated with the T cells. |
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