Unlike the ESP where there is an oversupply of older donors compared with older potential recipients, the number of older potential recipients far exceeds that of older donors in Australia. In 2008, there were 123 older potential recipients (aged ≥ 65 years) on the wait list compared with the availability of only 60 older donor kidneys (aged ≥ 65 years). Although there is a large discrepancy between the number of available donor kidneys
and wait-listed potential recipients across all donor and recipient age groups, there is a lesser difference at the extremes of donor and recipient age <35 and ≥65 years.7 One potential option of assimilating age-matching into the current allocation model may be to consider age-matching at the younger age group (i.e. all donor kidneys aged <35 years must be allocated to potential recipients aged <35 years), whilst acknowledging that a proportion of younger selleck chemicals llc recipients will mTOR inhibitor continue to receive older donor kidneys. A simulated statistical model comparing the outcomes of utility-based and the present allocation policies should be closely examined
before any changes are adopted into clinical practice. The continuing shortage of donor organs, coupled with the increased utilisation of marginal donor kidneys has rekindled the debate regarding adoption of an allocation system to maximize graft outcomes from available kidneys and increasing equity of access of potential recipients to deceased donor kidney transplantation. Although the appropriateness of adopting or integrating utility-based allocation into our current Dichloromethane dehalogenase allocation policy will generate enormous discussion among the transplant physicians,
surgeons and the community at large, preliminary modification to our current allocation model to optimize the use of our limited pool of deceased donor kidneys should be considered a priority. “
“Aim: Several proteins constituting the slit diaphragm are considered important for maintaining capillary wall permselectivity. Early intervention with blockers of angiotensin II receptors (AR) and mineralocorticoid receptors (MR) is effective against proteinuria in models of chronic hypertensive and protein-induced renal damage. However, the effects of AR and/or MR blockers in a model of acute nephrotic syndrome remain unknown. The effects of AR and MR blockers were examined in puromycin aminonucleoside (PAN)-treated rats. Methods: Six week old male Sprague–Dawley (SD) rats were injected with PAN or vehicle and assigned to groups as follows: vehicle (group C); PAN (group P); PAN followed 3 days later by administration of the MR blocker, eplerenone (group MR), and by the AR blocker, losartan (group AR). Blood pressure and urinary protein excretion were measured and all rats were killed for immunohistochemical investigation on day 14 after PAN administration. Results: Blood pressure did not change throughout the study period.