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CD8+ Cells Are Not Necessary for Allograft Rejection or the Induction of Apoptosis in an Experimental Model of Small Intestinal Transplantation

Allospecific CTL can function as cellular effectors of solid organ graft rejection; however, the specific mechanisms of cell damage remain undetermined. In this study we examined the role of CD8+ T cells in apoptosis and rejection of small intestinal allografts. ACI rat intestinal grafts transplante...

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Published in:	The Journal of immunology (1950) 1998-04, Vol.160 (8), p.3673-3680
Main Authors:	Krams, Sheri M, Hayashi, Michihiro, Fox, Christine K, Villanueva, Janeth C, Whitmer, Karen J, Burns, Washington, Esquivel, Carlos O, Martinez, Olivia M
Format:	Article
Language:	English
Subjects:	AIDS/HIV Animals Apoptosis - immunology CD8-Positive T-Lymphocytes - immunology Fas Ligand Protein fas Receptor - genetics Graft Rejection - etiology Graft Rejection - immunology Graft Rejection - pathology Granzymes Intestine, Small - immunology Intestine, Small - pathology Intestine, Small - transplantation Lymphocyte Depletion Male Membrane Glycoproteins - genetics Organ Transplantation Perforin Polymerase Chain Reaction Pore Forming Cytotoxic Proteins Rats Rats, Inbred ACI Rats, Inbred Lew Serine Endopeptidases - genetics Transplantation, Homologous
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description	Allospecific CTL can function as cellular effectors of solid organ graft rejection; however, the specific mechanisms of cell damage remain undetermined. In this study we examined the role of CD8+ T cells in apoptosis and rejection of small intestinal allografts. ACI rat intestinal grafts transplanted into Lewis rat recipients showed apoptosis of epithelial crypt cells on day 3 posttransplant as determined by terminal deoxynucleotidyl transferase-mediated deoxyuridine triphosphate nick end labeling staining. By day 7 numerous apoptotic crypt cells were detected in allografts, but were rarely observed in FK506-treated allograft recipients, isografts, or native intestine of allograft recipients. To further investigate the mechanism of rejection, recipient rats were depleted of CD8+ cells by treatment with OX-8 mAbs the day before and the day after transplantation of rat small intestinal allografts. Depletion of CD8+ cells from allograft recipients did not alter the tempo or the histologic features of rejection compared with those in the control (IgG-treated) group. Moreover, there was no difference in the number of apoptotic crypt epithelial cells in the grafts of control and CD8-depleted rats. Reverse transcriptase-PCR analyses determined there were similar levels of transcripts for Fas, Fas ligand, perforin, and granzyme B in control and CD8-depleted allograft recipients. By Western blot it was determined that the levels of Fas ligand protein were increased in the CD8-depleted group compared with those in control and FK506-treated allograft recipients. These data suggest that CD8 cells are not required for tissue injury or apoptotic cell death in small intestine allograft rejection.
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In this study we examined the role of CD8+ T cells in apoptosis and rejection of small intestinal allografts. ACI rat intestinal grafts transplanted into Lewis rat recipients showed apoptosis of epithelial crypt cells on day 3 posttransplant as determined by terminal deoxynucleotidyl transferase-mediated deoxyuridine triphosphate nick end labeling staining. By day 7 numerous apoptotic crypt cells were detected in allografts, but were rarely observed in FK506-treated allograft recipients, isografts, or native intestine of allograft recipients. To further investigate the mechanism of rejection, recipient rats were depleted of CD8+ cells by treatment with OX-8 mAbs the day before and the day after transplantation of rat small intestinal allografts. Depletion of CD8+ cells from allograft recipients did not alter the tempo or the histologic features of rejection compared with those in the control (IgG-treated) group. Moreover, there was no difference in the number of apoptotic crypt epithelial cells in the grafts of control and CD8-depleted rats. Reverse transcriptase-PCR analyses determined there were similar levels of transcripts for Fas, Fas ligand, perforin, and granzyme B in control and CD8-depleted allograft recipients. By Western blot it was determined that the levels of Fas ligand protein were increased in the CD8-depleted group compared with those in control and FK506-treated allograft recipients. 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In this study we examined the role of CD8+ T cells in apoptosis and rejection of small intestinal allografts. ACI rat intestinal grafts transplanted into Lewis rat recipients showed apoptosis of epithelial crypt cells on day 3 posttransplant as determined by terminal deoxynucleotidyl transferase-mediated deoxyuridine triphosphate nick end labeling staining. By day 7 numerous apoptotic crypt cells were detected in allografts, but were rarely observed in FK506-treated allograft recipients, isografts, or native intestine of allograft recipients. To further investigate the mechanism of rejection, recipient rats were depleted of CD8+ cells by treatment with OX-8 mAbs the day before and the day after transplantation of rat small intestinal allografts. Depletion of CD8+ cells from allograft recipients did not alter the tempo or the histologic features of rejection compared with those in the control (IgG-treated) group. Moreover, there was no difference in the number of apoptotic crypt epithelial cells in the grafts of control and CD8-depleted rats. Reverse transcriptase-PCR analyses determined there were similar levels of transcripts for Fas, Fas ligand, perforin, and granzyme B in control and CD8-depleted allograft recipients. By Western blot it was determined that the levels of Fas ligand protein were increased in the CD8-depleted group compared with those in control and FK506-treated allograft recipients. These data suggest that CD8 cells are not required for tissue injury or apoptotic cell death in small intestine allograft rejection.</description><subject>AIDS/HIV</subject><subject>Animals</subject><subject>Apoptosis - immunology</subject><subject>CD8-Positive T-Lymphocytes - immunology</subject><subject>Fas Ligand Protein</subject><subject>fas Receptor - genetics</subject><subject>Graft Rejection - etiology</subject><subject>Graft Rejection - immunology</subject><subject>Graft Rejection - pathology</subject><subject>Granzymes</subject><subject>Intestine, Small - immunology</subject><subject>Intestine, Small - pathology</subject><subject>Intestine, Small - transplantation</subject><subject>Lymphocyte Depletion</subject><subject>Male</subject><subject>Membrane Glycoproteins - genetics</subject><subject>Organ Transplantation</subject><subject>Perforin</subject><subject>Polymerase Chain Reaction</subject><subject>Pore Forming Cytotoxic Proteins</subject><subject>Rats</subject><subject>Rats, Inbred ACI</subject><subject>Rats, Inbred Lew</subject><subject>Serine Endopeptidases - genetics</subject><subject>Transplantation, Homologous</subject><issn>0022-1767</issn><issn>1550-6606</issn><fulltext>true</fulltext><rsrctype>article</rsrctype><creationdate>1998</creationdate><recordtype>article</recordtype><recordid>eNpNUctu1DAUtRCoTAtfgJC8gkWVwY5fyXI0lLZSKRKUteX40cnIiYPtaOAr-GUczbRidaV7Hrr3HADeYbSmiLaf9v0wzGPwa8zRulkTLsgLsMKMoYpzxF-CFUJ1XWHBxWtwntIeIcRRTc_AWctYg7hYgb_bz80l3FrvE9xEC-9DhvdW25RU_ANdiHDjfXiMymX43e6tzn0YYVnnnYW3o5lPCwc3U5hySH2C_QjVCK9-Tzb2gx2z8vBrMNYvrB-D8r4Is025HwvyENWYJq8KbXF6A1455ZN9e5oX4OeXq4ftTXX37fp2u7mrNBEiV04bbljLBcOaE6J5VztlHGUcKWramnaEtUKjGonOKS5Ea1xra0OJ6ahtDbkAH46-Uwy_5nKMHPqkSwxqtGFOUrQNxpThQiRHoo4hpWidnMpXJRyJkVxqkE81yFKDbORSQ1G9P9nP3WDNs-aUe8E_HvFd_7g79NHKtART2FgeDof_nP4B8O-VjQ</recordid><startdate>19980415</startdate><enddate>19980415</enddate><creator>Krams, Sheri M</creator><creator>Hayashi, Michihiro</creator><creator>Fox, Christine K</creator><creator>Villanueva, Janeth C</creator><creator>Whitmer, Karen J</creator><creator>Burns, Washington</creator><creator>Esquivel, Carlos O</creator><creator>Martinez, Olivia M</creator><general>Am Assoc Immnol</general><scope>CGR</scope><scope>CUY</scope><scope>CVF</scope><scope>ECM</scope><scope>EIF</scope><scope>NPM</scope><scope>AAYXX</scope><scope>CITATION</scope><scope>7X8</scope></search><sort><creationdate>19980415</creationdate><title>CD8+ Cells Are Not Necessary for Allograft Rejection or the Induction of Apoptosis in an Experimental Model of Small Intestinal Transplantation</title><author>Krams, Sheri M ; 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however, the specific mechanisms of cell damage remain undetermined. In this study we examined the role of CD8+ T cells in apoptosis and rejection of small intestinal allografts. ACI rat intestinal grafts transplanted into Lewis rat recipients showed apoptosis of epithelial crypt cells on day 3 posttransplant as determined by terminal deoxynucleotidyl transferase-mediated deoxyuridine triphosphate nick end labeling staining. By day 7 numerous apoptotic crypt cells were detected in allografts, but were rarely observed in FK506-treated allograft recipients, isografts, or native intestine of allograft recipients. To further investigate the mechanism of rejection, recipient rats were depleted of CD8+ cells by treatment with OX-8 mAbs the day before and the day after transplantation of rat small intestinal allografts. Depletion of CD8+ cells from allograft recipients did not alter the tempo or the histologic features of rejection compared with those in the control (IgG-treated) group. Moreover, there was no difference in the number of apoptotic crypt epithelial cells in the grafts of control and CD8-depleted rats. Reverse transcriptase-PCR analyses determined there were similar levels of transcripts for Fas, Fas ligand, perforin, and granzyme B in control and CD8-depleted allograft recipients. By Western blot it was determined that the levels of Fas ligand protein were increased in the CD8-depleted group compared with those in control and FK506-treated allograft recipients. These data suggest that CD8 cells are not required for tissue injury or apoptotic cell death in small intestine allograft rejection.</abstract><cop>United States</cop><pub>Am Assoc Immnol</pub><pmid>9558067</pmid><doi>10.4049/jimmunol.160.8.3673</doi><tpages>8</tpages><oa>free_for_read</oa></addata></record>
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subjects	AIDS/HIV Animals Apoptosis - immunology CD8-Positive T-Lymphocytes - immunology Fas Ligand Protein fas Receptor - genetics Graft Rejection - etiology Graft Rejection - immunology Graft Rejection - pathology Granzymes Intestine, Small - immunology Intestine, Small - pathology Intestine, Small - transplantation Lymphocyte Depletion Male Membrane Glycoproteins - genetics Organ Transplantation Perforin Polymerase Chain Reaction Pore Forming Cytotoxic Proteins Rats Rats, Inbred ACI Rats, Inbred Lew Serine Endopeptidases - genetics Transplantation, Homologous
title	CD8+ Cells Are Not Necessary for Allograft Rejection or the Induction of Apoptosis in an Experimental Model of Small Intestinal Transplantation
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