These patients underwent open surgical exploration through a midline transperitoneal or a flank retroperitoneal approach. In both approaches,
kidney mobilization outside the Gerota’s fascia, temporal renal pedicle clamping and partial nephrectomy or renorrhaphy were done in AC220 mouse a stepwise manner. Results: During the study period, we had 8 patients for whom angioembolization had failed (n = 4), was not available (n = 2) or the patient could not afford it (n = 2). Median patients’ age was 31 years (range 16-59 years). We did a partial nephrectomy in 2 and renorrhaphy in 6 of patients with a successful outcome. Median operative time was 2.25 h and median warm ischemia time was 26 min (range 24-42 min). After a median follow up period of 21 months, the involved renal unit, in all cases, remained functional in the postoperative intravenous urography. Conclusion: Massive hemorrhage after PCNL when angioembolization failed or was not feasible due to any reason could be controlled by partial nephrectomy or renorrhaphy with
the same principles as that used for surgical exploration in patients with FK866 in vitro high grade renal trauma. (C) 2014 Surgical Associates Ltd. Published by Elsevier Ltd. All rights reserved.”
“INTRODUCTION. Assessing blood-donor haemoglobin (Hb) is a worldwide screening requirement against inappropriate donation. The pre-donation Hb (which should be at least 12.5 g/dL in women and 13.5 g/dL in men) is usually determined in capillary blood from a finger prick,
using a spectrophotometer which reveals Acalabrutinib the absorbance of blood haemolysed in a microcuvette. New non-invasive methods of measuring Hb are now available. MATERIALS AND METHODS. In the first semester of 3 consecutive years three different strategies were employed to screen donors for anaemia at the moment of donation. In 2011 all whole-blood donors underwent the finger-prick method using azide-methaemoglobin: the test’s negative predictive value (NPV) was determined by comparison with the sub-threshold Hb values ascertained by haemocytometry of test-tube blood drawn at the start of the donation. In 2012 the donor evaluation was based on NBM 200 occlusion spectrophotometry. The same approach was kept in 2013, but a haemocytometry test was added on a pre-donation venous sample drawn from donors who, though fit to donate, had previous critical Hb values in their clinical records. RESULTS. In 2011, the NPV (in 3,856 donors) was 86% for women and 95% for men; in 2012 (3,966 donors), the values were 85% and 95%, respectively, and in 2013 (3,995 donors) they were 91% and 97%, respectively. Fisher’s test for contingency tables revealed no statistically significant differences between 2011 and 2012, but the 2013 results were a significant improvement. DISCUSSION.