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Dive into the research topics where Scott Kaczmorski is active.

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Featured researches published by Scott Kaczmorski.


The review of diabetic studies : RDS | 2011

Pancreas transplantation: lessons learned from a decade of experience at Wake Forest Baptist Medical Center.

Jeffrey Rogers; Alan C. Farney; S. Al-Geizawi; Samy S. Iskandar; William Doares; Michael D. Gautreaux; Lois J. Hart; Scott Kaczmorski; A. Reeves-Daniel; S. Winfrey; Mythili Ghanta; Patricia L. Adams; Robert J. Stratta

This article reviews the outcome of pancreas transplantations in diabetic recipients according to risk factors, surgical techniques, and immunosuppression management that evolved over the course of a decade at Wake Forest Baptist Medical Center. A randomized trial of alemtuzumab versus rabbit anti-thymocyte globulin (rATG) induction in simultaneous kidney-pancreas transplantation (SKPT) at our institution demonstrated lower rates of acute rejection and infection in the alemtuzumab group. Consequently, alemtuzumab induction has been used exclusively in all pancreas transplantations since February 2009. Early steroid elimination has been feasible in the majority of patients. Extensive experience with surveillance pancreas biopsies in solitary pancreas transplantation (SPT) is described. Surveillance pancreas biopsy-directed immunosuppression has contributed to equivalent long-term pancreas graft survival rates in SKPT and SPT recipients at our center, in contrast to recent registry reports of persistently higher rates of immunologic pancreas graft loss in SPT. Furthermore, the impact of donor and recipient selection on outcomes is explored. Excellent results have been achieved with older (extended) donors and recipients, in recipients of organs from donation after cardiac death donors managed with extracorporeal support, and in African-American patients. Type 2 diabetics with detectable C-peptide levels have been transplanted successfully with outcomes comparable to those of insulinopenic diabetics. Our experiences are discussed in the light of findings reported in the literature.


Expert Opinion on Biological Therapy | 2014

Depleting antibody induction in simultaneous pancreas-kidney transplantation: a prospective single-center comparison of alemtuzumab versus rabbit anti-thymocyte globulin

Robert J. Stratta; Jeffrey Rogers; Giuseppe Orlando; Umar Farooq; Yousef Al-Shraideh; William Doares; Scott Kaczmorski; Alan C. Farney

Background: The study purpose was to analyze midterm outcomes in a prospective trial of alemtuzumab (Alem) versus rabbit anti-thymocyte globulin (rATG) induction in simultaneous pancreas-kidney transplantation (SPKT). Methods: From February 2005 to October 2008, 46 SPKTs (45 portal-enteric drainage) were prospectively randomized as part of a larger kidney transplant study to receive either single-dose Alem (30 mg intraoperatively) or multiple-dose rATG antibody induction (starting intraoperatively, minimum three doses administered) with tacrolimus/mycophenolate ± steroids. Results: Of 222 kidney transplant patients enrolled in the study, 46 received SPKTs; 28 (61%) received Alem and 18 (39%) rATG induction. Follow-up ranged from 67 to 111 months (mean 80 months). There were no significant differences between the two groups in 5 years actual patient (86% Alem vs 89% rATG), kidney (82% Alem vs 61% rATG, p = 0.17) or pancreas (68% Alem vs 56% rATG) graft survival rates. Five years death-censored kidney (92% Alem vs 69% rATG, p = 0.09) and pancreas (76% Alem vs 56% rATG, p = 0.198) graft survival rates were slightly higher in patients receiving Alem. Acute rejection (21% Alem vs 44% rATG, p = 0.12) and major infection (39% Alem vs 67% rATG, p = 0.13) rates were slightly lower in the Alem group; cytomegalovirus infections were significantly lower (0 Alem vs 17% rATG, p = 0.05). The incidence of late acute rejection was low in both groups. There were no differences in early pancreas thrombosis (3.6% Alem vs 11% rATG), postoperative bleeding (11% Alem vs 0 rATG), other surgical complications, readmissions or freedom from steroids between groups. In patients with functioning grafts, 5 years mean serum creatinine (1.4 Alem vs 1.6 mg/dl rATG), calculated abbreviated modification of diet in renal disease glomerular filtration rate (55 Alem vs 52 ml/min/1.73 m2 rATG), hemoglobin A1c (both 5.4%) and C-peptide (2.6 Alem vs 2.3 ng/ml rATG) levels were similar. Conclusions: Single-dose Alem and multiple-dose rATG induction provide similar midterm patient survival and graft functional outcomes with no major differences in morbidity or resource utilization.


Clinical Transplantation | 2016

Dual kidney transplants from adult marginal donors successfully expand the limited deceased donor organ pool

Robert J. Stratta; Alan C. Farney; Giuseppe Orlando; Umar Farooq; Yousef Al-Shraideh; Amudha Palanisamy; A. Reeves-Daniel; William Doares; Scott Kaczmorski; Michael D. Gautreaux; Samy S. Iskandar; Gloria Hairston; Elizabeth Brim; Margaret Mangus; Hany El-Hennawy; Muhammad Arsalan Khan; Jeffrey Rogers

The need to expand the organ donor pool remains a formidable challenge in kidney transplantation (KT). The use of expanded criteria donors (ECDs) represents one approach, but kidney discard rates are high because of concerns regarding overall quality. Dual KT (DKT) may reduce organ discard and optimize the use of kidneys from marginal donors.


Clinical Transplantation | 2014

Influence of recipient age on deceased donor kidney transplant outcomes in the expanded criteria donor era

Yousef Al-Shraideh; Umar Farooq; Alan C. Farney; Amudha Palanisamy; Jeffrey Rogers; Giuseppe Orlando; Michael R. Buckley; A. Reeves-Daniel; William Doares; Scott Kaczmorski; Michael D. Gautreaux; Samy S. Iskandar; Gloria Hairston; Elizabeth Brim; Margaret Mangus; Robert J. Stratta

We performed a retrospective single‐center review of 884 deceased donor (DD) kidney transplants (KTs) in patients (pts) aged ≥40 yr.


World journal of transplantation | 2016

Single vs dual (en bloc) kidney transplants from donors ≤ 5 years of age: A single center experience

Yousef Al-Shraideh; Umar Farooq; Hany El-Hennawy; Alan C. Farney; Amudha Palanisamy; Jeffrey Rogers; Giuseppe Orlando; Muhammad Saif Ullah Khan; A. Reeves-Daniel; William Doares; Scott Kaczmorski; Michael D. Gautreaux; Samy S. Iskandar; Gloria Hairston; Elizabeth Brim; Margaret Mangus; Robert J. Stratta

AIM To compare outcomes between single and dual en bloc (EB) kidney transplants (KT) from small pediatric donors. METHODS Monocentric nonprospective review of KTs from pediatric donors ≤ 5 years of age. Dual EB KT was defined as keeping both donor kidneys attached to the inferior vena cava and aorta, which were then used as venous and arterial conduits for the subsequent transplant into a single recipient. Donor age was less useful than either donor weight or kidney size in decision-making for kidney utilization as kidneys from donors < 8 kg or kidneys < 6 cm in length were not transplanted. Post-transplant management strategies were standardized in all patients. RESULTS From 2002-2015, 59 KTs were performed including 34 dual EB and 25 single KTs. Mean age of donors (17 mo vs 38 mo, P < 0.001), mean weight (11.0 kg vs 17.4 kg, P = 0.046) and male donors (50% vs 84%, P = 0.01) were lower in the dual EB compared to the single KT group, respectively. Mean cold ischemia time (21 h), kidney donor profile index (KDPI; 73% vs 62%) and levels of serum creatinine (SCr, 0.37 mg/dL vs 0.49 mg/dL, all P = NS) were comparable in the dual EB and single KT groups, respectively. Actuarial graft and patient survival rates at 5-years follow-up were comparable. There was one case of thrombosis resulting in graft loss in each group. Delayed graft function incidence (12% dual EB vs 20% single KT, P = NS) was slightly lower in dual EB KT recipients. Initial duration of hospital stay (mean 5.4 d vs 5.6 d) and the one-year incidences of acute rejection (6% vs 16%), operative complications (3% vs 4%), and major infection were comparable in the dual EB and single KT groups, respectively (all P = NS). Mean 12 mo SCr and abbreviated MDRD levels were 1.17 mg/dL vs 1.35 mg/dL and 72.5 mL/min per 1.73 m(2) vs 60.5 mL/min per 1.73 m(2) (both P = NS) in the dual EB and single KT groups, respectively. CONCLUSION By transplanting kidneys from young pediatric donors into adult recipients, one can effectively expand the limited donor pool and achieve excellent medium-term outcomes.


Transplantation | 2011

Gout and Transplantation: New Treatment Option—same Old Drug Interaction

Scott Kaczmorski; William Doares; S. Winfrey; S. Al-Geizawi; Alan C. Farney; Jeffrey Rogers; Robert J. Stratta

The authors declare no conflict of interest. Address correspondence to: Jing-yu Chen, M.D., Lung Transplantation Group, Wuxi People’s Hospital, Nanjing Medical University, Room A516, 299 Qing Yang Road, Wuxi, Jiangsu 214000, China. E-mail: [email protected] D.W. and J.-Y.C. participated in research design; D.W., F.G., and T.B. participated in the writing of the manuscript; and D.W., M.-F.Z., S.-G.Y., F.L., Y.-H.Z., B.W., J.Z., and J.-Y.C. participated in the performance of the research. Received 7 March 2011. Revision requested 19 March 2011. Accepted 23 April 2011. Copyright


Case reports in nephrology | 2015

Donor-Derived Myeloid Sarcoma in Two Kidney Transplant Recipients from a Single Donor

Amudha Palanisamy; Paul Persad; Patrick P. Koty; Laurie L. Douglas; Robert J. Stratta; Jeffrey Rogers; A. Reeves-Daniel; Giuseppe Orlando; Alan C. Farney; Michael W. Beaty; Mark J. Pettenati; Samy S. Iskandar; David D. Grier; Scott Kaczmorski; William Doares; Michael D. Gautreaux; Barry I. Freedman; Bayard L. Powell

We report the rare occurrence of donor-derived myeloid sarcoma in two kidney transplant patients who received organs from a single deceased donor. There was no evidence of preexisting hematologic malignancy in the donor at the time of organ recovery. Both recipients developed leukemic involvement that appeared to be limited to the transplanted organ. Fluorescence in situ hybridization (FISH) and molecular genotyping analyses confirmed that the malignant cells were of donor origin in each patient. Allograft nephrectomy and immediate withdrawal of immunosuppression were performed in both cases; systemic chemotherapy was subsequently administered to one patient. Both recipients were in remission at least one year following the diagnosis of donor-derived myeloid sarcoma. These cases suggest that restoration of the immune system after withdrawal of immunosuppressive therapy and allograft nephrectomy may be sufficient to control HLA-mismatched donor-derived myeloid sarcoma without systemic involvement.


Journal of gerontology and geriatric research | 2016

Deceased Donor Kidney Transplantation in Patients Aged 70 and Older: Is 70 the New 50?

Umar Farooq; Yousef Al-Shraideh; Alan C. Farney; Amudha Palanisamy; Jeffrey Rogers; Giuseppe Orlando; A. Reeves-Daniel; William Doares; Scott Kaczmorski; Hany El-Hennawy; Muhammad Saif Ullah Khan; Michael D. Gautreaux; Samy S. Iskandar; Gloria Hairston; Elizabeth Brim; Robert J. Stratta

Background: Deceased donor (DD) kidney transplantation (KT) outcomes in patients who are aged 70 years and older are understudied. Methods: We retrospectively reviewed our single center DD KT outcomes in patients aged 70 years and older. All patients received antibody induction with tacrolimus, half-dose mycophenolate, ± steroids. Results: Over 10.75 years, we performed 114 KTs in 112 patients aged 70 and older (mean 73.8, range 70-84 years) including 42 patients who were aged 75 and older. The study group included 60 males/52 females and 79 Caucasians/28 African Americans/5 other with a mean waiting time of 16 months; 75 patients (66%) received kidneys from expanded criteria donors (ECDs) and 14 received dual KTs. Delayed graft function occurred in 27% and influenced graft but not patient survival. With a mean follow-up of 68 months, patient survival was 59% and uncensored kidney graft survival was 47%. Three year and death-censored kidney graft survival rates were 76% and 74%, respectively. Outcomes were similar in patients < or ≥ 75 years. Of 60 graft losses, death with a functioning graft (DWFG) accounted for 41 (68%). Of 46 deaths, 72% were due to cardio/cerebrovascular events, infection, or malignancy. At present, 54 of the 66 surviving patients (81.8%) have functioning grafts. The incidences of acute rejection and major infection were 14% and 45%, respectively. Conclusions: Advanced recipient age has a modest effect on medium-term outcomes in appropriately selected elderly patients using predominantly ECD kidneys, which may not be appropriate for younger patients. However, medium-term outcomes are largely influenced by a higher incidence of DWFGs in the elderly, suggesting that matching strategies for kidney and patient longevity are warranted.


Clinical Transplantation | 2017

Analysis of local versus imported expanded criteria donor kidneys: A single-center experience with 497 ECD kidney transplants

Muhammad Arsalan Khan; Hany El-Hennawy; Alan C. Farney; Jeffrey Rogers; Giuseppe Orlando; A. Reeves-Daniel; Amudha Palanisamy; Michael D. Gautreaux; Samy S. Iskandar; William Doares; Scott Kaczmorski; Robert J. Stratta

The value of importing expanded criteria donor (ECD) kidneys is uncertain.


Clinical Transplantation | 2018

Is prolonged cold ischemia a contraindication to using kidneys from acute kidney injury donors

Giuseppe Orlando; Muhammad Arsalan Khan; Hany El-Hennawy; Alan C. Farney; Jeffrey Rogers; A. Reeves-Daniel; Michael D. Gautreaux; William Doares; Scott Kaczmorski; Robert J. Stratta

To determine the impact of prolonged cold ischemia time (CIT) on the outcome of acute kidney injury (AKI) renal grafts, we therefore performed a single‐center retrospective analysis in adult patients receiving kidney transplantation (KT) from AKI donors. Outcomes were stratified according to duration of CIT. A total of 118 patients receiving AKI grafts were enrolled. Based on CIT, patients were stratified as follows: (i) <20 hours, 27 patients; (ii) 20‐30 hours, 52 patients; (iii) 30‐40 hours, 30 patients; (iv) ≥40 hours, nine patients. The overall incidence of delayed graft function DGF was 41.5%. According to increasing CIT category, DGF rates were 30%, 42%, 40%, and 78%, respectively (P = .03). With a mean follow‐up of 48 months, overall patient and graft survival rates were 91% and 81%. Death‐censored graft survival (DCGS) rates were 84% and 88% for patients with and without DGF (P = NS). DCGS rates were 92% in patients with CIT <20 hours compared to 85% with CIT >20 hours (P = NS). In the nine patients with CIT >40 hours, the 4‐year DCGS rate was 100%. We conclude that prolonged CIT in AKI grafts may not adversely influence outcomes and so discard of AKI kidneys because of projected long CIT is not warranted when donors are wisely triaged.

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Robert J. Stratta

Wake Forest Baptist Medical Center

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