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1 te allografts (VCAs; a.k.a. composite tissue allotransplantation).
2 the potential of the BM as a site for islet allotransplantation.
3 lementation of paediatric vascular composite allotransplantation.
4 timulatory pathway to a murine model of limb allotransplantation.
5 aft-versus-host disease and recurrence after allotransplantation.
6 s on the inflammatory processes triggered by allotransplantation.
7 ising combination for clinical evaluation in allotransplantation.
8 ns for the immunotherapy of autoimmunity and allotransplantation.
9 ay be equally applicable to composite-tissue allotransplantation.
10 d to the development of OAD following airway allotransplantation.
11 on plays a role in the poor success of islet allotransplantation.
12 an primate models of autoimmune diseases and allotransplantation.
13 erivative (RAD), in cynomolgus monkey kidney allotransplantation.
14 solution to the shortage of donor organs for allotransplantation.
15 in a rat hindlimb model of composite tissue allotransplantation.
16 mune-mediated diseases and for outcome after allotransplantation.
17 zation, prior LVAD support, or prior cardiac allotransplantation.
18 l after anti-CD25 induction therapy in islet allotransplantation.
19 in patients (n = 29) who had undergone lung allotransplantation.
20 ne reactivity, when placed in the context of allotransplantation.
21 a promising agent for clinical use in human allotransplantation.
22 le additional risk involved with parathyroid allotransplantation.
23 dness and is a major complication of corneal allotransplantation.
24 most common donor-associated infection after allotransplantation.
25 t survival in the murine model of orthotopic allotransplantation.
26 ic those arising during MHC mismatched human allotransplantation.
27 ransplantation as a practical alternative to allotransplantation.
28 d the risk/benefit balance in bilateral hand allotransplantation.
29 rapy might improve graft survival in cardiac allotransplantation.
30 etic with streptozotocin and underwent islet allotransplantation.
31 to play a significantly greater role than in allotransplantation.
32 confirmed acceptance of PSCs in MHC-matched allotransplantation.
33 tment of rejection in vascularized composite allotransplantation.
34 duction, immunosuppressive therapy, or islet allotransplantation.
35 play a significant role in composite tissue allotransplantation.
36 pproximate the antibody binding occurring in allotransplantation.
37 to address the shortage of human organs for allotransplantation.
38 m deceased individuals continues to restrict allotransplantation.
39 ection after ABO-compatible HLA-incompatible allotransplantation.
40 an outbred non-human primate model of renal allotransplantation.
41 ascular arterial thrombosis in murine aortic allotransplantation.
42 ngle surgical procedure using composite face allotransplantation.
43 tion under stress conditions such as cardiac allotransplantation.
44 de as well as for the graft to survive after allotransplantation.
45 nimum theoretical standard to work toward in allotransplantation.
46 lymphoid tissues as early as 3 h post-islet allotransplantation.
47 ly being investigated in a clinical trial of allotransplantation.
48 ffering new perspectives in composite tissue allotransplantation.
49 in vivo, in models of alloimmune priming and allotransplantation.
50 body formation during the early period after allotransplantation.
51 framework for approaching the endothelium in allotransplantation.
52 on the restoration of facial deformities by allotransplantation.
53 nsplanted along with islets during auto- and allotransplantations.
55 ational Society on Hand and Composite Tissue Allotransplantation, a section of The Transplantation So
56 unosuppression in mice 30 days before aortic allotransplantation across C57Bl/ 10J (H2b)-->C3H (H2k)
59 the first report suggestive of CR in a face allotransplantation after immunosuppression minimization
60 er a pig xenograft would preclude subsequent allotransplantation, although the data available suggest
63 is study, we extended our regimen to cardiac allotransplantation and compared the immunological respo
64 ejection and could potentially be applied to allotransplantation and prevention of the autoimmune rec
65 ndent cellular cytotoxicity, to human AMR in allotransplantation and xenotransplantation and illustra
66 ght reduce subsequent acute rejection, after allotransplantation, and coronary allograft vasculopathy
67 (MHC) are the primary barrier to successful allotransplantation, and here we describe class I MHC mo
68 recipients of successful intrahepatic islet allotransplantation, and in matched control subjects.
69 assist device (LVAD) support, prior cardiac allotransplantation, and pulmonary hypertension, are und
72 evidence that autoimmune responses following allotransplantation are damaging and cause accelerated g
74 , support the continued application of islet allotransplantation as a treatment modality for type 1 d
77 have use as an adjunctive agent for clinical allotransplantation, but using the dosing regimens we us
78 Before a human clinical trial of hepatocyte allotransplantation can be attempted, preliminary experi
79 ), whereas Karnofsky scores less than 90% at allotransplantation correlated with shorter PFS only (P
81 Numerous experiments in composite tissue allotransplantation (CTA) have identified skin as the mo
86 deal model to study various composite tissue allotransplantation (CTA)-related problems, we designed
89 ALB/c and NOD mice and that successful islet allotransplantation depends on the degree of hyperglycem
91 n = 4) who underwent facial composite tissue allotransplantation (FCTA) at our center between April 2
92 sion is being developed as a bridge to liver allotransplantation for patients with fulminant hepatic
93 mples from patients awaiting cadaveric renal allotransplantation for reactivity against: 1) human; 2)
96 tes after heterotopic partial facial segment allotransplantation from major histocompatibility comple
99 Although heterologous vascular composite allotransplantation has become a burgeoning treatment op
103 pite technical feasibility, composite tissue allotransplantation has not been applied clinically beca
104 nic rejection (CR) in vascularized composite allotransplantation has not been included in the Banff c
106 in the supply of human organs available for allotransplantation has turned attention toward the use
107 menon repeats itself after second same donor allotransplantation, hoping to determine whether accepta
108 he widespread clinical use of reconstructive allotransplantation if protocols to achieve this could b
109 allotransplantation was inaugurated by hand allotransplantation in 1998, giving rise to many controv
111 lts in clinical trials, in contrast to islet allotransplantation in animal models, which have demonst
113 in contrast to clinical experience with AB-I allotransplantation in infants, who cease producing only
117 good tolerability in a preclinical model of allotransplantation in nonhuman primates and thus has in
118 monoclonal antibody (hu5C8) allows for renal allotransplantation in outbred, MHC-mismatched rhesus mo
119 doses of corticosteroid hormones after renal allotransplantation in the era of cyclosporine and tacro
120 emonstrate that immune tolerance after organ allotransplantation in the rat is associated with a repr
121 poglycemia and 2) whether intrahepatic islet allotransplantation in type I diabetic patients and cons
123 st that activation of donor T cells after SB allotransplantation induces production of a Th1-like pro
127 between bone marrow transplantation and limb allotransplantation is required, making such protocols i
128 ined HLA-matched donor bone marrow and renal allotransplantation is the first example of an intention
131 on of graft survival after intraportal islet allotransplantation (ITx) in rats: 7.2 days in the contr
132 human cytomegalovirus (HCMV) infection after allotransplantation led us to evaluate whether baboon cy
133 yeloablative preconditioning and barriers to allotransplantation limit this therapy to children with
135 natives to the current technology of cardiac allotransplantation may include xenotransplantation and/
136 plants using nonmyeloablative regimens (mini-allotransplantations) may hold promise for more widely e
137 mobilized and collected T cells, which after allotransplantation, might positively affect the inciden
139 minates this delay period in a rat hind limb allotransplantation model by performing mixed allogeneic
140 a non-human primate facial composite tissue allotransplantation model to investigate strategies to a
142 on with cyclosporine (CsA) in a rat hindlimb allotransplantation model with a major antigenic mismatc
145 to prevent graft rejection in a mouse heart allotransplantation model; the highest dose tested (1.5
147 p 1 Cynomolgus monkeys (n=6) underwent TIR + allotransplantation of hematopoietic cells and a kidney
151 ble immune tolerance supporting vascularized allotransplantation offers the possibility of extending
153 d in 64 liver transplant patients, 59 kidney allotransplantation patients and six lung transplant pat
154 The study included 5 cases of bilateral hand allotransplantation performed in a single center, with a
155 ecurrence rates were 21%, 43%, and 58% after allotransplantation, purged autotransplantation, and unp
156 ory receptors on T cells and modification of allotransplantation regimens have all produced new tumor
160 Ischemia times in vascularized composite allotransplantation should be kept as short as possible
162 together, our results suggest that following allotransplantation, T cell responses to donor antigens
163 In July, 2015, our vascularised composite allotransplantation team did the first bilateral hand an
164 trategy for tolerance induction in laryngeal allotransplantation that permits escape from chronic imm
165 n this study, using a murine model of aortic allotransplantation, the role of blockade of signaling t
168 e our initial experience with abdominal wall allotransplantation to facilitate abdominal closure.
171 r immunomodulation in vascularized composite allotransplantation (VCA) have gained importance due to
172 imate model of facial vascularized composite allotransplantation (VCA) to study the association of Tr
173 y induce tolerance in vascularized composite allotransplantation (VCA) with chimerism through bone ma
175 ng process for vascularized composite tissue allotransplantation (VCTA) closely follows the standard
181 Using a well-characterized model of corneal allotransplantation, we demonstrate in this study that T
182 th research on penile vascularized composite allotransplantation will require the articulation of gui
186 in preventing acute rejection in adult liver allotransplantation with less renal toxicity and less us
188 aluated in19 monkeys that underwent auto- or allotransplantation, with or without subtherapeutic immu
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