The influence of primary non-function on the accuracy of ultrasound measurements in the diagnosis of renal allograft rejection

Nicholson, Michael L.; Bell, A.; Donnelly, P. K.; Veitch, P. S.; Bell, P. R. F.

doi:10.1007/bf00337101

Cited by 1 publication

(1 citation statement)

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“…Recipients of syngeneic skin also showed a marked reduction in graft inflammation after treatment with mtCCL7 for 2 days. This may have important clinical implications as ischemia-reperfusion is a major cause of inflammation and graft nonfunction (25); 5-10% of liver allografts show primary nonfunction, whilst for renal allografts an incidence of 32% has been reported (26).…”

Section: Discussionmentioning

confidence: 99%

Therapy with Nonglycosaminoglycan‐Binding Mutant CCL7: A Novel Strategy to Limit Allograft Inflammation

Ali

O'Boyle

Hepplewhite

et al. 2010

American Journal of Transplantation

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Chemokines are immobilized by binding to glycosaminoglycans (GAGs). A non-GAG-binding mutant CCL7 (mtCCL7) was developed that retained its affinity for chemokine receptors. This mtCCL7 induced leukocyte chemotaxis in diffusion gradients but did not stimulate trans-endothelial migration (p < 0.01). Unlike wild-type CCL7, mtCCL7 persisted in the circulation of BALB/c mice for more than 6 h and prevented leukocyte infiltration of skin isografts (p < 0.05). Treatment with mtCCL7 marginally increased the survival of C57BL/6 to BALB/c skin allografts and reduced graft infiltration by CD3 + cells (p < 0.05). Importantly, mtCCL7 promoted long-term (>40 day) graft survival following minor histocompatibility (HY) antigen mismatched C57BL/6 skin transplantation; control grafts were rejected by day 24. Treatment with mtCCL7 produced a significant decrease in the frequency of IFN-c producing donor-reactive splenic T cells, reduced CCR2 expression by circulating leukocytes for 6 h (p < 0.01) and blocked the normal increase in affinity of a 4b 1 integrins for VCAM-1 following transient chemokine stimulation. These data suggest that mtCCL7 persists in the circulation and reduces both specific T-cell priming and the capacity of circulating immune cells to respond to GAG-bound chemokine at sites of developing inflammation.

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Section: Discussionmentioning

confidence: 99%