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1. |
RECURRENT GLOMERULONEPHRITIS FOLLOWING RENAL TRANSPLANTATION |
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Transplantation,
Volume 63,
Issue 8,
1997,
Page 1045-1052
Kotanko1,2 Peter,
Pusey Charles,
Levy3 Jeremy,
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ISSN:0041-1337
出版商:OVID
年代:1997
数据来源: OVID
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2. |
T-CELL COSTIMULATORY BLOCKADE IN EXPERIMENTAL CHRONIC CARDIAC ALLOGRAFT REJECTIONEffects of Cyclosporine and Donor Antigen1 |
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Transplantation,
Volume 63,
Issue 8,
1997,
Page 1053-1058
Chandraker Anil,
Russell Mary,
Glysing-Jensen Troels,
Willett Theresa,
Sayegh2 Mohamed,
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摘要:
Chronic rejection is a T cell-dependent process and blockade of the CD28-B7 T-cell costimulatory activation pathway by the fusion protein CTLA4Ig has been shown to prevent the development of accelerated graft arteriosclerosis in a rat model of chronic cardiac allograft rejection. The effectiveness of T-cell costimulatory blockade at preventing chronic allograft rejection in a clinically relevant model in combination with cyclosporine therapy has not been investigated. Using the well-established LEW into F334 heterotopic cardiac allograft model, we show that when cyclosporine is administered in combination with CTLA4Ig, it abrogates the previously demonstrated protective effect of CTLA4Ig in preventing chronic allograft rejection. Long-term surviving allografts from animals treated with a combination of cyclosporine and CTLA4Ig had a mean vascular luminal occlusion of 42.2%, affecting more than 90% of graft vessels due to accelerated arteriosclerosis. This was associated with up-regulation of intragraft expression of mRNA for CD4, the costimulatory molecule B7, the T-cell cytokine interferon-γ, monocyte chemoattractant protein-1, and the fibrogenic growth factor transforming growth factor-β; all have been previously shown to be associated with development of chronic rejection in this model. In comparison, the addition of donor splenocytes to the combination of CTLA4Ig and cyclosporine therapy protocol significantly reduced the amount of arteriosclerosis; mean vascular luminal occlusion was 11.3%, affecting approximately 50% of vessels. This was associated with decreased intragraft expression of CD4, B7, interferon-γ, monocyte chemoattractant protein-1, and transforming growth factor-β. These data indicate that the mechanism of action of CTLA4Ig in attenuating chronic rejection is cyclosporine sensitive, and that strategies implying combination of CTLA4Ig and cyclosporine may not be clinically desirable. Administration of donor antigen may be necessary if CTLA4Ig and cyclosporine are to be combined, to prevent the process of chronic rejection.
ISSN:0041-1337
出版商:OVID
年代:1997
数据来源: OVID
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3. |
BONE FORMATION IN VIVO: COMPARISON OF OSTEOGENESIS BY TRANSPLANTED MOUSE AND HUMAN MARROW STROMAL FIBROBLASTS |
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Transplantation,
Volume 63,
Issue 8,
1997,
Page 1059-1069
Krebsbach1,2 Paul,
Kuznetsov3 Sergei,
Satomura3 Kazuhito,
Emmons4 Robert,
Rowe5 David,
Robey3,6 Pamela,
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摘要:
Background.Marrow stromal fibroblasts (MSFs) are known to contain bone precursor cells. However, the osteogenic potential of human MSFs has been poorly characterized. The aim of this study was to compare the osteogenic capacity of mouse and human MSFs after implantation in vivo.Methods.After in vitro expansion, MSFs were loaded into a number of different vehicles and transplanted subcutaneously into immunodeficient mice.Results.Mouse MSFs transplanted within gelatin, polyvinyl sponges, and collagen matrices all formed a capsule of cortical-like bone surrounding a cavity with active hematopoiesis. In transplants of MSFs from transgenic mice harboring type I procollagen-chloramphenicol acetyltransferase constructs, chloramphenicol acetyltransferase activity was maintained for up to 14 weeks, indicating prolonged bone formation by transplanted MSFs. New bone formation by human MSFs was more dependent on both the in vitro expansion conditions and transplantation vehicles. Within gelatin, woven bone was observed sporadically and only after culture in the presence of dexamethasone and L-ascorbic acid phosphate magnesium salt n-hydrate. Consistent bone formation by human MSFs was achieved only within vehicles containing hydroxyapatite/tricalcium phosphate ceramics (HA/TCP) in the form of blocks, powder, and HA/TCP powder-type I bovine fibrillar collagen strips, and bone was maintained for at least 19 weeks. Cells of the new bone were positive for human osteonectin showing their donor origin. HA/TCP powder, the HA/TCP powder-type I bovine fibrillar collagen strips, and HA/TCP powder held together with fibrin were easier to load and supported more extensive osteogenesis than HA/TCP blocks and thus may be more applicable for therapeutic use.Conclusions.In this article, we describe the differences in the requirements for mouse and human MSFs to form bone, and report the development of a methodology for the consistent in vivo generation of extensive bone from human MSFs.
ISSN:0041-1337
出版商:OVID
年代:1997
数据来源: OVID
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4. |
L-ARGININE AND ALLOPURINOL PROTECT AGAINST CYCLOSPORINE NEPHROTOXICITY1 |
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Transplantation,
Volume 63,
Issue 8,
1997,
Page 1070-1073
Assis2 Sônia,
Monteiro José,
Seguro Antonio,
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摘要:
The role of nitric oxide (NO) and oxygen free radicals in cyclosporine (CsA) nephrotoxicity was investigated using L-arginine, an NO substrate, and allopurinol, a xanthine oxidase inhibitor (involved in the formation of oxygen radicals) in an experimental model with Wistar rats. CsA, administered at 15 mg/kg/body weight (BW) subcutaneously for 10 days, caused a decrease in glomerular filtration rate, with inulin clearance of 0.33±0.04 vs. 1.11±0.06 ml/min/100 g BW (P<0.01 vs. control). L-Arginine, 1.5% in drinking water 5 days before and during CsA administration, partially protected the animals against this fall in glomerular filtration rate, with inulin clearance of 0.68±0.03 ml/min/100 g BW (P<0.01 vs. CsA). Allopurinol, at 10 mg/kg/BW by gavage, also had a protective action, with inulin clearance of 0.54±0.04 ml/min/100 g (P<0.01 vs. CsA). CsA caused an elevation in NO production, as assessed by urinary excretion of its metabolities, nitrite and nitrate (NO2and NO3; 0.836±0.358 vs. 0.107±0.019 nmol/μg creatinine). NO production was as much as threefold higher in the L-arginine group (1.853±0.206 nmol/g creatinine). This CsA effect is probably related to its vasoconstrictive stimulus. Supplementation with L-arginine, which provides more substrate for NO formation, may enhance vasodilatation and consequently reduce the impairment of renal function. The protection provided by allopurinol may be related to the reduced formation of oxygen radicals, preventing the deleterious effects of lipid peroxidation.
ISSN:0041-1337
出版商:OVID
年代:1997
数据来源: OVID
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5. |
A CONTROLLED ANALYSIS OF THE TRANSJUGULAR INTRAHEPATIC PORTOSYSTEMIC SHUNT IN LIVER TRANSPLANT RECIPIENTS |
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Transplantation,
Volume 63,
Issue 8,
1997,
Page 1074-1079
Somberg1,2 Kenneth,
Lombardero3 Manuel,
Lawlor3 Sharon,
Ascher4 Nancy,
Lake1 John,
Wiesner5 Russell,
Zetterman6 Rowen,
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摘要:
Background.The transjugular intrahepatic portosystemic shunt (TIPS) is an important treatment for complications of portal hypertension. As some authors have suggested that TIPS may facilitate liver transplantation technically, the objective of this study was to determine the impact of TIPS on the liver transplant operation and its outcome.Methods.The analysis was designed as a retrospective cohort study using a multicenter database. Fifty-five patients with TIPS were matched with 55 controls on the basis of 10 pretransplant laboratory, clinical, and demographic features. TIPS patients and control patients were compared with regard to duration of surgery, intraoperative blood product usage, liver and renal function, volume of ascites, survival, and hospital stay. For confirmatory purposes, a parallel analysis using linear regression methods was performed.Results.By matched analysis, TIPS patients had less ascites at surgery (mean 0.9±0.20 vs. 2.2±0.37 L,P=0.005) and a slightly shorter time from incision to cross-clamp (mean 2.1±0.10 vs. 2.5±0.15 hr,P=0.03). However, there were not significant differences for total operative time (mean 6.0±0.17 vs. 6.3±0.25 hr,P=1.00), blood product usage, or any other outcome variable. Regression analysis confirmed these results.Conclusions.TIPS does not significantly impact the course of liver transplantation surgery. Therefore, preoperative portal decompression solely to facilitate liver transplantation is not an appropriate indication for TIPS.
ISSN:0041-1337
出版商:OVID
年代:1997
数据来源: OVID
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6. |
IDIOPATHIC PNEUMONIA SYNDROMEChanging Spectrum of Lung Injury after Marrow Transplantation1 |
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Transplantation,
Volume 63,
Issue 8,
1997,
Page 1079-1086
Kantrow2 Stephen,
Hackman Robert,
Boeckh Michael,
Myerson David,
Crawford3 Stephen,
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摘要:
Background.The aim of our study was to describe the incidence, clinical course, and risk factors for the idiopathic pneumonia syndrome (IPS), compared with those previously described for “idiopathic pneumonia,” after bone marrow transplantation (BMT).Methods.Our study design was a case-series review with determination of risk by comparison with unaffected controls by log-rank or Fisher's exact (two-tailed) test and logistic regression analyses. The study group comprised 1165 consecutive marrow recipients at a single center from 1988 to 1991.Results.IPS was documented in 85 BMT recipients (7.3%) by bronchoalveolar lavage (n=68), open lung biopsy (n=3), or autopsy (n=14). The calculated actuarial incidence for IPS within 120 days after BMT was 7.7%. Median time to onset was 21 days (mean 34±30). Hospital mortality was 74%, and 53 BMT recipients (62%) died with progressive respiratory failure. IPS resolved in 22 patients (26%); 18 patients (21%) survived to discharge. Mechanical ventilation was required by 59 BMT recipients (69%), within a median of 2 days of onset of infiltrates. Two of these 59 recipients (3%) survived to discharge. Pulmonary infection (predominantly fungal) was noted in 7 of 25 (28%) BMT recipients who had an autopsy. Potential risk factors for IPS were assessed in univariate and multivariate logistic regression analyses. Although the incidence was not significantly different between autologous (5.7%) and allogeneic marrow recipients (7.6%), risks were identified only for the latter: malignancy other than leukemia (odds ratio=6.5 compared with aplastic anemia), and grade 4 graft-versus-host disease (odds ratio=5.4 compared with lower grades). No factors were associated with recovery.Conclusions.The incidence of idiopathic lung injury seems lower, the onset earlier, and the risk factors different from those previously reported. The major risks seem to be regimen-related toxicity and multiorgan dysfunction associated with alloreactive processes.
ISSN:0041-1337
出版商:OVID
年代:1997
数据来源: OVID
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7. |
MURINE OKT4A IMMUNOSUPPRESSION IN CADAVER DONOR RENAL ALLOGRAFT RECIPIENTSA Cooperative Clinical Trials in Transplantation Pilot Study1 |
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Transplantation,
Volume 63,
Issue 8,
1997,
Page 1087-1095
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摘要:
Background.A phase I study of anti-CD4 immunosuppression of cadaver donor renal allograft recipients was conducted by the NIH Cooperative Clinical Trials in Transplantation to assess safety, tolerability, immunoactivity, and pharmacokinetics of multiple infusions of murine anti-human CD4 monoclonal antibody OKT4A.Methods.Thirty patients were enrolled (August 1992 to October 1993) and received OKT4A at dosages of 0.5 mg/kg (24 patients), 1.0 mg/kg (3 patients), and 2.0 mg/kg (3 patients), beginning and continuing for 12 consecutive days with a standard regimen of cyclosporine, azathioprine, and prednisone. OKT4A treatment was continued after surgery if serum creatinine 24 hr after transplantation was <85% of pretransplantation baseline creatinine.Results.Ninety-three percent of patients treated at 0.5 mg/kg OKT4A and all patients at higher doses had mean peak CD4 saturations in excess of 90%. A human anti-mouse antibody response of >3 times pretreatment levels was observed in 84% of patients. There was no evidence of CD4 T cell depletion. OKT4A was well tolerated without first-dose side effects. For the 19 eligible patients treated with 0.5 mg/kg OKT4A with initial graft function, the 3-month treated rejection rate was 37%. The 2-year graft survival rate for all 30 patients enrolled was 83%, and for the 19 eligible patients, 95%.Conclusions.The high percentage of CD4 saturation, the minimal side effects, the observation of a low 3-month rejection rate, and an excellent 2-year graft survival rate in patients treated with 0.5 mg/kg OKT4A support the continued investigation of an anti-CD4 approach to immunosuppressive therapy.
ISSN:0041-1337
出版商:OVID
年代:1997
数据来源: OVID
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8. |
INHIBITION OF INDUCIBLE NITRIC OXIDE SYNTHASE AMELIORATES FUNCTIONAL AND HISTOLOGICAL CHANGES OF ACUTE LUNG ALLOGRAFT REJECTION1,2 |
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Transplantation,
Volume 63,
Issue 8,
1997,
Page 1095-1101
Worrall3,4 Neil,
Boasquevisque4 Carlos,
Botney5 Mitchell,
Misko6 Thomas,
Sullivan7 Patrick,
Ritter8 Jon,
Ferguson4 T.,
Patterson4,9 G.,
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摘要:
Background.We recently demonstrated that inhibition of inducible nitric oxide synthase (iNOS) ameliorated severe acute lung allograft rejection. This study used a rat lung transplant model to determine (1) the time course and cellular localization of iNOS expression during the histological progression of unmodified acute rejection and (2) whether inhibition of iNOS prevented impaired gas exchange function of the allograft lung and/or ameliorated the histological changes of acute rejection.Methods and Results.iNOS mRNA and enzyme activity were expressed in allograft lungs during mild, moderate, and severe acute rejection, but not in normal, isograft, or allograft lungs before histological changes of mild acute rejection. iNOS expression in allografts resulted in elevated serum nitrite/nitrate levels, indicative of increased in vivo nitric oxide (NO) production. In situ hybridization demonstrated iNOS mRNA expression in infiltrating inflammatory cells, but not in allograft parenchymal cells. Allografts had significantly impaired gas exchange, which was prevented with the selective iNOS inhibitor aminoguanidine (PaO2of 566±19, 76±22, and 504±105 mmHg for isograft, allograft, and aminoguanidine-treated allograft, respectively;P<0.0002). Aminoguanidine also significantly improved the histological rejection scores.Conclusions.(1) iNOS expression and increased NO production occurred during the early stages of acute rejection, persisted throughout the unmodified rejection process, and localized to infiltrating inflammatory cells, but not allograft parenchymal cells; (2) aminoguanidine ameliorated the histological and functional changes of acute rejection; and (3) increased NO production, detected by the presence of iNOS mRNA, protein, or noninvasively by measuring serum nitrite/nitrate levels, may serve as an early marker of acute allograft rejection.
ISSN:0041-1337
出版商:OVID
年代:1997
数据来源: OVID
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9. |
SEQUENTIAL CELLULAR AND MOLECULAR KINETICS IN ACUTELY REJECTING RENAL ALLOGRAFTS IN RATS1 |
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Transplantation,
Volume 63,
Issue 8,
1997,
Page 1101-1108
Nagano2 Hiroaki,
Nadeau2,3 Kari,
Takada2 Moriatsu,
Kusaka2 Mamoru,
Tilney2,4 Nicholas,
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摘要:
The initial (0-24 hr), early (3-5 days), and late (7-14 days) events occurring in LBNF1 renal allografts transplanted into Lew recipients were examined to define precisely the sequential cellular and molecular kinetics during acute rejection. Grafts and spleens were harvested at 3, 6, 12, and 24 hr, and at 3, 5, 7, and 14 days and processed for morphology, immunohistology, and reverse transcriptase-polymerase chain reaction. Various factors (mRNA) were up-regulated sequentially in the allografts over time. In the initial phase, E-selectin and complement (C1 and C3) expression was noted within 6 hr, peaking by 24 hr. RANTES (regulated upon activation, normal T cell expressed and secreted) increased within 6 hr, and then again between 3 and 6 days. By immunohistology, MHC class II was up-regulated consistently after day 1. Intercellular adhesion molecule-1 expression increased after day 3; lymphocyte function-associated antigen-1+infiltrating leukocytes peaked at day 5. Infiltrating CD8+T lymphocytes increased strikingly between days 1 and 3, peaking at day 5; CD4+cells infiltrated more slowly until day 5. The kinetics of ED1+macrophages were similar to those of lymphocyte function-associated antigen-1+cells. The CD4+T cell-derived product, interleukin (IL)-2, peaked at 7 days. Interferon-γ increased progressively up to 14 days. By 3 days, the macrophage-associated factor, transforming growth factor-β, peaked; this was followed by increased IL-6 expression by day 5. IL-1, tumor necrosis factor-α, and inducible nitric oxide synthase increased slowly until day 7, declining thereafter. Endothelin increased progressively over the 14-day follow-up period. Cytokine dynamics occurring in host spleen were similar to those noted in the allografts.Although acute rejection is primarily T cell mediated, adhesion molecules, macrophages, and their associated products may influence initial and later changes. The brisk expression of complement, E-selectin, and RANTES within the first few hours after engraftment may occur secondary to ischemic injury and trigger subsequent immunological events. Macrophages and their products may play a larger role in the process than hitherto appreciated.
ISSN:0041-1337
出版商:OVID
年代:1997
数据来源: OVID
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10. |
PROLONGED MURINE CARDIAC ALLOGRAFT ACCEPTANCECharacteristics of Persistent Active Alloimmunity after Treatment with Gallium Nitrate Versus Anti-CD4 Monoclonal Antibody1,2 |
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Transplantation,
Volume 63,
Issue 8,
1997,
Page 1109-1117
Orosz3,4,5,6 Charles,
Wakely3 Elaine,
Sedmak6 Daniel,
Bergese3 Sergio,
VanBuskirk3 Anne,
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摘要:
We have treated DBA/2→C57BL/6 murine cardiac allograft recipients with anti-CD4 monoclonal antibody or with gallium nitrate to promote long-term (>60 days) allograft survival. Within this period, all grafts developed histologic evidence of ongoing vascular and parenchymal tissue remodeling, including interstitial fibrosis and neointimal hyperplasia, which are characteristic of chronic allograft rejection. To evaluate residual alloimmunity associated with the pharmacologic avoidance of acute graft rejection and the development of chronic tissue remodeling, we subjected these graft recipients to a battery of histologic and immunologic tests. Similar test results were obtained for graft recipients treated with either of the two immunosuppressive agents. All long-surviving allografts displayed histologic evidence of ongoing microvascular endothelial activation and interstitial leukocytic infiltration. Reverse transcriptase-polymerase chain reaction analyses demonstrated intragraft expression of mRNAs for interleukin (IL)-1, IL-2, IL-4, IL-6, tumor necrosis factor, interferon-γ, and transforming growth factor-β. All recipients had limiting dilution analysis-detectable, graft-reactive cytolytic T lymphocytes and helper T lymphocytes in their spleens and grafts, and all produced high titers of graft-reactive alloantibodies. In general, these observations indicate that (1) a similar immune status is achieved in long-surviving allografts and their recipients when either anti-CD4 monoclonal antibody or gallium nitrate was used for antirejection therapy, (2) this immune status is characterized by continuous, long-term inflammatory and immune processes that are qualitatively similar to those observed during acute allograft rejection, and (3) no specific immune responses developed selectively in long-term graft recipients to account for the avoidance of acute graft rejection or the development of chronic tissue remodeling in the graft.
ISSN:0041-1337
出版商:OVID
年代:1997
数据来源: OVID
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