Structural and physical studies of the lipopolysaccharide antigens from Pseudomonas aeruginosa /

Riley, David Alan

January 1981

No description available.

Chemistry

Lipopolysaccharides

Antigens

Pseudo aeruginosa

Regulatory cell interactions following the oral administration of antigen /

Domen, Patricia Louise

January 1984

No description available.

Health Sciences

Cell interaction

Antigens

Structural and immunological studies of the lipopolysaccharide antigens of pseudomonas aeruginosa /

Schweitzer, Mark Glenn

January 1984

No description available.

Chemistry

LIPOPOLYSACCHARIDES

Antigens

Pseudo aeruginosa

Studies on the stable antigens of African trypanosomes : Serodiagnosis of Trypanosoma congolense infection of rabbits by the latex fixation test /

Mahmoud, Mahmoud Musa,1940-

January 1970

No description available.

Biology

Antigens

Rabbits

Trypanosoma congolense

Bovine semen iso-antigens : detection, determination of origin and partial characterization by immunological, physico-chemical and electro-phoretic methods /

Mellad, Kirkland Earle

January 1974

No description available.

Health Sciences

Antigens

Semen

Cattle

Immune responses to skin xenografts and extraction of xenotransplantation antigens /

Hines, David Lee

January 1975

No description available.

Health Sciences

Transplantation immunology

Antigens

Immunological and biochemical characterization of feline oncornavirus-induced tumor antigens /

Wolff, Linda Heding

January 1977

No description available.

Biology

Oncogenic viruses

Tumor antigens

Characterization of a T lymphocyte-derived, antigen-binding molecule with suppressive activity

Chu, Nelson Randall

January 1989

Regulation of the immune response is mediated, in part, by the action of suppressor T cells (Ts). One intriguing aspect of these cells is the description of T cell suppressor factor (TsF): a soluble analog of the cell that shares many of its properties, such as the ability to bind free antigen (Ag) and suppress an Ag-specific immune response. The exact molecular nature of TsF and the relationship of TsF to Ts are unknown. The immune response to the small, bacterial protein, ferredoxin (Fd), was used as a model system to study TsF. A Fd-specific suppressor cell network has been described in mice that are genetically nonresponsive to this Ag. Previously, a soluble mediator, known as Fd11F, was found in the culture supernatant (SN) of the Ts hybridoma, Fd11. Fd11F possessed both Ag-binding activity and the ability to suppress the anti-Fd Ab response in mice. The TsF-specific monoclonal antibody, B16G, was used for both the recovery of Fd11F-enriched material from SN and its detection by the enzyme-linked immunosorbent assay. ' Further immunochemical, biological, and biochemical characterization of Fd11F was done with emphasis on describing the Ag-binding properties of Fd11F. It was found that Fd11F bound to solid- and liquid-phase Fd, and demonstrated preferential binding to the carrier determinant of the Ag. A spleen cell culture assay was devised which showed that Fd11F suppressed Ab production in a concentration-dependent manner. Additional experiments suggested that the suppressive effect was Ag-specific. The identification of the Ag-binding molecule was attempted by the fractionation of Fd11F-enriched material using high performance gel filtration or preparative SDS-PAGE (run under non-reducing conditions). Using SDS-PAGE, a unique, single polypeptide of about 30k relative molecular mass (Mr) was identified as the Ag-binding moiety of Fd11F. The possible relationship of this moiety to other identified materials is discussed. / Science, Faculty of / Microbiology and Immunology, Department of / Graduate

T cells

Antigens

Suppressor cells

Antigens, Differentiation, T-Lymphocyte

Antigens -- immunology

Suppressor cells -- immunology

Characterization and cDNA cloning of a novel murine T cell surface antigen YE1/48

Chan, Po-Ying

January 1988

T cell surface antigens are thought to play significant roles in immunological functions. They are involved in cellular interactions and T cell activation and proliferation. Characterization of T cell antigens is important in understanding the molecular machanisms underlying immune responses. The subject of this thesis is to characterize a novel murine T cell surface antigen called YE1/48. YE1/48, defined by two rat monoclonal antibodies YE1/48.10.6 and YE1/32.8.5, is a dimeric glycoprotein with molecular size and charge resembling the murine T cell antigen receptor α/β. It was initially detected at high levels on two T cell lymphomas, EL-4 and MBL-2. In my thesis studies, the YE1/48 antigen was characterized biochemically, a cDNA clone was isolated, and its expression in lymphoid cell populations was determined. The YE1/48 antigen was found to be distinct from the T cell receptor based on direct comparisons of their primary sequences as well as immunological analyses. It is likely a homodimer with similar or identical subunits. No homology with any known proteins could be detected, including the human T cell activation antigen CD28 (T44) which also has a similar dimeric structure as YE1/48. No function of the YE1/48 antigen could be derived from its primary sequence or with the use of the two monoclonal antibodies because the antibodies do not appear to bind to the surface of intact normal T lymphocytes. Some intriguing characteristics of the YE1/48 antigen were observed in the current studies. The YE1/48 antigen belongs to a rare group of type II membrane proteins with orientation of the amino-terminus inside the cell and the carboxy-terminus outside. The YE1/48 gene may have two alleles among different mouse strains and may belong to a multigene family. YE1/48 is expressed at low levels on a wide range of T cells with no restriction to their differentiation stages, and on spleen B cells as well as bone marrow cells. Its expression on lymphocytes is not related to activation or proliferation. However, YE1/48 expression appears to be induced at high levels by Abelson Murine Leukemia Virus-transformation of pre-B cells. Moreover, the epitopes defined by the YE1/48.10.6 and YE1.32.8.5 antibodies seem to be exposed only on three T lymphomas but not on normal T cells. It is thus tantalizing to speculate a correlation of the high level expression of YE1/48 antigen and its epitope exposure on transformed lymphocytes with cellular transformation. In summary, YE1/48 was found to be a novel T cell surface antigen which has similar dimeric structure as the murine T cell receptor α/β and human CD28 (T44). It has now been characterized biochemically, molecularly cloned, and its expression on lymphoid cells has been determined. Although the function of YE1/48 antigen remains unknown, a number of intriguing characteristics observed in the current studies have certainly called for further studies on the antigen and the determination of its function. / Science, Faculty of / Microbiology and Immunology, Department of / Graduate

T cells

Antigens, Surface

Cell surface antigens

Antigens, Differentiation, T-Lymphocyte

Induction and regulation of bovine B lymphocyte responses

Haas, Karen M.

January 2000

Thesis (Ph. D.)--University of Missouri--Columbia, 2000. / Typescript. Vita. Includes bibliographical references (leaves 177-206). Also available on the Internet.