Chronic rejection in rat aortic allografts. An experimental model for transplant arteriosclerosis.

Mennander, Ari; Tiisala, Sinikka; Halttunen, Jorma; Yılmaz, Serdar; Paavonen, Timo; Häyry, P

doi:10.1161/01.atv.11.3.671

Cited by 191 publications

(108 citation statements)

References 12 publications

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“…The correlation between adventitial infiltration by inflammatory cells and the ratio of intimal proliferation to medial thickness in untreated allografts demonstrates one of the major features of the model, the importance of inflammation in the injury and response to chronic vascular immune aggression. Nevertheless, Mennander et al 7 reported that adventitial inflammation was predominant during the first month after arterial grafting in this model, a time when medial smooth muscle cells were still present. After this time, the adventitial inflammation decreased in parallel with the disappearance of medial smooth muscle cells.…”

Section: Discussionmentioning

confidence: 69%

“…The evidence of rejection probably decreases in untreated allografts in relation to the disappearance of smooth muscle cellular antigens 2 months after grafting. 7 In contrast, low doses of cyclosporin could delay the appearance of rejection, so that the inflammation appeared greater in cyclosporin-treated animals than in untreated allografts 2 months after grafting. This inflammation could be related to the persistence of medial cellular antigens, as suggested by the positive correlation between medial smooth muscle cell and adventitial inflammatory cell densities.…”

Section: Discussionmentioning

confidence: 99%

See 1 more Smart Citation

Additive and synergistic effects of a low-molecular-weight, heparin-like molecule and low doses of cyclosporin in preventing arterial graft rejection in rats.

Plissonnier

Amichot

Lecagneux

et al. 1993

Arterioscler Thromb

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Arteriosclerotic intimal proliferation is one of the main long-term complications of organ transplantation. Low-molecular-weight, heparin-like molecules prevent myointimal proliferation in arterial wall injury and limit rejection in skin allografts. Cyclosporin limits rejection but has no major effect on intimal proliferation. Therefore, an experimental protocol was designed to test whether heparin-like molecules interacted with low doses of cyclosporin to prevent arterial wall immune system injury and response in a model of arterial graft rejection in normotensive and hypertensive rats. Aortic allografts were performed in spontaneously hypertensive rats (SHRs) and Wistar-Kyoto (WKY) normotensive control rats. Four groups of 10 allografted (SHR and WKY) rats were used: one group was treated with placebo, one with low doses of cyclosporin (2 nig/kg body wt per day), one with low-molecular-weight, heparin-like molecule (1 nig/kg body wt per hour), and one with low doses of cyclosporin plus low-molecular-weight, heparin-like molecule. Ten SHRs and 10 WKYs were isografted and served as the control groups. All rats were killed 8 weeks after aortic grafting. Structural parameters of the grafted segment were measured by morphometric analysis on formalin-fixed sections with specific stains. The classical signs of immune system injury and response were present in the untreated allografts in SHRs and WKYs: inflammatory infiltration of the adventitia, medial injury, and intimal proliferative response. Low doses of cyclosporin had a significant beneficial effect on immune medial injury by increasing medial thickness and the number of remaining smooth muscle cells and decreasing the extracellular matrix injury. Cyclosporin had no protective effect on intimal proliferation. Low-molecularweight, heparin-like molecules had a beneficial effect on both the medial injury and the intimal proliferative response that was independent of blood pressure. Heparin-like molecules increased medial thickness and partially prevented smooth muscle cell loss and extracellular matrix attack. They also significantly decreased the intimal thickness by acting more on the collagen content than on the smooth muscle cell density. Low doses of cyclosporin plus heparin-like molecules had a marked effect in preventing the arterial wall injury and response. This combination resulted in a normal medial appearance, increased medial thickness and smooth muscle cell number, and no intimal proliferation or adventitial inflammation. Thus, heparin-like molecules appear to act in concert with low doses of cyclosporin in preventing rejection-induced arterial wall remodeling in an experimental model of aortic allograft in rats, and their effects are independent of blood pressure. (Arteriosclerosis and Thrombosis 1993;13:112-119)

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Section: Discussionmentioning

confidence: 69%

Section: Discussionmentioning

confidence: 99%

Additive and synergistic effects of a low-molecular-weight, heparin-like molecule and low doses of cyclosporin in preventing arterial graft rejection in rats.

Plissonnier

Amichot

Lecagneux

et al. 1993

Arterioscler Thromb

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“…Our group first showed (32) that MPA is able to reduce the incidence and severity of GVD in a Brown Norway-to-Lewis transplant model. In addition, MMF reduced the obliteration of renal arteries at a dose of 15 mg/kg/day (33) that no initial immunosuppressive therapy is needed to secure graft function (34,35) and GVD can be investigated independently. In an ACI-to-Lewis model of orthotopic aortic transplantation, intimal proliferation was reduced by 76.1% with the daily treatment of 40-30 mg/kg MMF (8).…”

Section: Discussionmentioning

confidence: 99%

Treatment by Mycophenolate Mofetil of Advanced Graft Vascular Disease in Non‐Human Primate Recipients of Orthotopic Aortic Allografts

Klupp¹,

Dambrin²,

Hibi³

et al. 2003

American Journal of Transplantation

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Failure to control chronic graft dysfunction [e.g. graft vascular disease (GVD)] is the primary cause of immunologic graft failure. This is the first study of mycophenolate mofetil (MMF) for the treatment of GVD in non-human primate recipients of aortic allografts. Abdominal aortic allografts were exchanged between mixed leukocyte reaction (MLR) -mismatched, blood-group-compatible cynomolgus monkeys. Six control recipients were untreated. Individualized treatment with frequent dose adjustments of MMF insured that treatment was close to the maximum tolerated dose (mean 99.2 mg/kg/day). Immune-mediated injury proceeded unhindered until day 45, after which MMF treatment began. Changes in intimal volume (IV) were quantified by intravascular ultrasound (IVUS) and compared to histology on day 105. Serial IVUS measurements of IV (mm 3 ) in controls showed progressive GVD. In four out of six animals, MMF was well tolerated, thus enabling optimum treatment; in all these animals, IV was significantly less than in the control animals (p = 0.02). In the two remaining animals, high doses were not tolerated; at day 105, there was no significant difference in IV between them and the controls. We found a significant correlation between the mean MMF tolerated dose and the inhibition of progression of IV (r = À0.88, p = 0.015). When high MMF doses were tolerated, MMF slowed progression of GVD.

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“…Consequently arterial allografts have generally been transplanted without considering the matching of AB0-bloodgroups and of HLA-phenotypes between donors and recipients. Furthermore, only a limited number of studies exist which have investigated the allo-specific immune response induced by arterial allografts, and the majority of them is based on animal models [12][13][14][15][16]. There are only few studies mainly of the 1990s in which the cellular and humoral immune responses as a consequence of venous and especially arterial allo-grafting in humans was investigated [8,[17][18][19][20].…”

Section: Introductionmentioning

confidence: 99%

Strong Humoral Anti-HLA Immune Response Upon Arbitrarily Chosen Allogeneic Arterial Vessel Grafts

H¹,

Wahle²,

Altermann³

et al. 2017

J Clin Cell Immunol

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Forty-three patients were grafted with forty-four fresh or cryopreserved allogeneic arterial vessels in order to treat infections of synthetic vascular implants as these often lead to sepsis, amputation and death. All the patients were HLA-typed whereas typing results of the post-mortem donors were inquired or genotyped from residuary vessels' segments. 84% of the patients were cured from the underlying infections with a re-infection rate of only 9% attesting this therapeutic procedure a high success rate for recovering from the bacterial infections. Since the allografts were chosen without considering HLA-histocompatibility between donors and recipients 95% of the patients developed a humoral anti-HLA immune response with 89% of them giving rise to virtually definable donor-specific antibodies. Regarding the clinical outcome 16% of the patients exhibited thromboses as the most frequent complication. In addition to clinical follow up analyses of all patients, tissue excisions of 11 patients' allografts due to various complications but not resulting from persisting infections were analyzed in order to compare these vessels' pre-and post-transplant histological appearance. In contrast to three early excised homografts (after 14 to 45 days) all of the later on explanted vessels (after 8 to 96 months) clearly showed chronic degeneration processes induced by the alloreactive immune response. Although not leading to acute graft dysfunctions comparable to those of solid organs, arbitrarily selected vessels exhibit a high degree of alloimmunization with consequent chronic degeneration processes such as the loss of smooth muscle cells. Additionally, clear signs of fibrosis of the different arterial vessel layers lead to obliterative arteriopathy and thromboses. Thus, apparently the overall practicability of the unmatched allocation of arterial homografts is clearly limited. Further approaches of arterial vessel allo-grafting are required to investigate the hypothesis that the clinical outcome of well HLA-matched homografts may lead to a significantly decreased number of thromboses.

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Chronic rejection in rat aortic allografts. An experimental model for transplant arteriosclerosis.

Cited by 191 publications

References 12 publications

Additive and synergistic effects of a low-molecular-weight, heparin-like molecule and low doses of cyclosporin in preventing arterial graft rejection in rats.

Additive and synergistic effects of a low-molecular-weight, heparin-like molecule and low doses of cyclosporin in preventing arterial graft rejection in rats.

Treatment by Mycophenolate Mofetil of Advanced Graft Vascular Disease in Non‐Human Primate Recipients of Orthotopic Aortic Allografts

Strong Humoral Anti-HLA Immune Response Upon Arbitrarily Chosen Allogeneic Arterial Vessel Grafts

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