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Dive into the research topics where M. Francesca Egidi is active.

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Featured researches published by M. Francesca Egidi.


Transplantation | 1998

LONG-TERM RESULTS OF PANCREAS TRANSPLANTATION UNDER TACROLIMUS IMMUNOSUPPRESSION

Mark L. Jordan; Ron Shapiro; H. Albin Gritsch; M. Francesca Egidi; Ajai Khanna; Carlos Vivas; Velma P. Scantlebury; John J. Fung; Thomas E. Starzl; Robert J. Corry

Background The long-term safety and efficacy of tacrolimus in pancreas transplantation has not yet been demonstrated. The observation of prolonged pancreatic graft function under tacrolimus would indicate that any potential islet toxicity is short-lived and clinically insignificant. We report herein the results of pancreas transplantation in patients receiving primary tacrolimus immunosuppression for a minimum of 2 years. Methods. From July 4, 1994 until April 18, 1996, 60 patients received either simultaneous pancreas-kidney transplant (n=55), pancreas transplant only (n=4), or pancreas after kidney transplantation (n=1). Baseline immunosuppression consisted of tacrolimus and steroids without antilymphocyte induction. Azathioprine was used as a third agent in 51 patients and mycophenolate mofetil in 9. Rejection episodes within the first 6 months occurred in 48 (80%) patients and were treated with high-dose corticosteroids. Antilymphocyte antibody was required in eight (13%) patients with steroid-resistant rejection. Results. With a mean follow-up of 35.1±5.9 months (range: 24.3-45.7 months), 6-month and 1-, 2-, and 33-year graft survival is 88%, 82%, 80%, and 80% (pancreas) and 98%, 96%, 93%, and 91% (kidney), respectively. Six-month and 1-, 2-, and 3-year patient survival is 100%, 98%, 98%, and 96.5%. Mean fasting glucose is 91.6±13.8 mg/dl, and mean glycosylated hemoglobin is 5.1±0.7% (normal range: 4.3-6.1%). Mean tacrolimus dose is 6.5±2.6 mg/day and mean prednisone dose 2.0±2.9 mg/day at follow-up. Complete steroid withdrawal was possible in 31 (65%) of the 48 patients with functioning pancreases. Conclusions. These data show for the first time that tacrolimus is a safe and effective long-term primary agent in pancreas transplantation and provides excellent long-term islet function without evidence of toxicity while permitting steroid withdrawal in the majority of patients.


Transplantation | 1995

Combined simultaneous kidney/bone marrow transplantation.

Ron Shapiro; Abdul S. Rao; Paulo Fontes; Adrianna Zeevi; Mark L. Jordan; Velma P. Scantlebury; Carlos Vivas; H. Albin Gritsch; Robert J. Corry; M. Francesca Egidi; Maria T. Rugeles; H. L. R. Rilo; Abdelouahab Aitouche; Anthony J. Demetris; G. Rosner; Massimo Trucco; Witold Rybka; William Irish; John J. Fung; Thomas E. Starzl

On the basis of observations in patients with long-term (28-30 years) renal allograft survival, all of whom had evidence of systemic microchimerism, we began a program of combined simultaneous kidney/bone marrow transplantation. Between 12/14/92, and 10/31/94, 36 kidney transplant recipients received 3-5 x 10(8) unmodified bone marrow cells/kg; 6 patients also received pancreatic islets, and 7 patients also received a pancreas. The mean recipient age was 39.0 +/- 10.8 years, and the mean donor age was 31.8 +/- 16.1 years; the mean cold ischemia time was 23.0 +/- 9.1 hr. Twenty control patients received kidneys alone, mainly because of refusal by the donor family to consent to vertebral body recovery; 3 of these patients also received a pancreas. The mean recipient age was 47.9 +/- 11.7 years, and the mean donor age was 41.5 +/- 17.9 years; the mean cold ischemia time was 28.6 +/- 6.2 hr. All patients received tacrolimus-based therapy, without radiation, cytoreduction, or induction antilymphocyte preparations. Blood was drawn prior to and at regular intervals after transplantation for detection of chimerism and for immunologic studies. With a mean follow-up of 11.1 +/- 5.8 months, all 36 study patients are alive, and 33 (92%) have functioning allografts with a mean serum creatinine of 1.9 +/- 1.2 mg/dl and a BUN of 26 +/- 9 mg/dl. Graft vs. host disease was not seen in any patient. The incidence of rejection was 72%; 11% of the patients required OKT3 or ATG for steroid-resistant rejection. The incidence of CMV was 14%, and that of delayed graft function was 17%. A total of 18 (90%) control patients are alive, and 17 (85%) have functioning allografts, with a mean serum creatinine of 2.1 +/- 1.3 mg/dl, and a BUN of 30 +/- 13 mg/dl. The incidence of rejection was 60%, and 10% required OKT3 or ATG. CMV was seen in 15%, and delayed graft function in 20% (P = NS). In the study patients, chimerism was detected in the peripheral blood of 30 of 31 (97%) evaluable patients by either PCR or flow cytometry. In the control patients, chimerism was seen in 9 of 14 (64%) evaluable patients (P < .02). Decreasing donor-specific responsiveness was seen in 6/29 (21%) evaluable study, and 4/14 (29%) evaluable control patients (P = NS). We conclude that combined kidney/bone marrow transplantation is associated with acceptable patient and graft survival, augmentation of chimerism, and no change in the early events after transplantation.


Transplantation | 1997

Spontaneous arterioenteric fistula after pancreas transplantation.

H. Albin Gritsch; Ron Shapiro; M. Francesca Egidi; Parmjeet Randhawa; Thomas E. Starzl; Robert J. Corry

Chronic pancreas transplant rejection with enteric exocrine drainage can lead to significant long-term complications. We report a case of a 47-year-old male insulin-dependent diabetic who survived the complications of peripancreatic abscess, enterocutaneous fistula, and arterioenteric fistula related to pancreas transplantation. To avoid these long-term complications, we now recommend elective removal of nonfunctioning, enterically drained pancreas allografts.


Clinical Transplantation | 2000

Outcomes of simultaneous kidney-pancreas transplantation in African-American recipients: a case-control study.

Agnes Lo; Robert J. Stratta; M. Francesca Egidi; M. Hosein Shokouh-Amiri; Hani P. Grewal; A. Tarik Kizilisik; Rita R. Alloway; Lillian W. Gaber; A. Osama Gaber

Introduction. Previous studies have suggested that African‐American (AA) ethnicity is a risk factor for rejection and graft loss after kidney transplantation. However, little data is available regarding outcomes after simultaneous kidney–pancreas transplantation (SKPT) in AA recipients. The objective of this study was to compare the outcomes of SKPT in AA patients to matched Caucasian patients as controls. u2028Methods. From January 1996 to September 1999, we performed 79 SKPTs, including 10 in AA recipients. Ten Caucasian controls were selected and matched for age, gender, weight, timing and technique of transplantation, and immunosuppressive regimen. Clinical outcomes were collected and compared between the two groups. u2028Results. The two groups were well matched for donor and recipient demographic, immunologic and transplant characteristics, including 2 patients in each group with type 2 diabetes. All patients received tacrolimus (TAC), mycophenolate mofetil (MMF) and steroids, and about half in each group received antibody induction therapy. Patient survival was 100% in both groups with a mean follow‐up of 18 months (range 6–47). Kidney and pancreas graft survival rates were both 80% in the AA and 100% in the Caucasian groups, respectively (p=0.14). All but one kidney (in the AA group) and all pancreas grafts experienced immediate function. There were two immunologic kidney and two immunologic pancreas graft losses in the AA group. No grafts were lost due to technical problems. The mean length of initial hospital stay was 16 d in the AA group compared to 10 d in the Caucasian group (p=0.07). The AA group had a slight increase in the number of readmissions (mean 2.2 AA vs. 1.6 Caucasian, p=0.08). The incidence of biopsy‐proven pancreas acute rejection was significantly higher in the AA group (50%) compared to the Caucasian group (10%) (p=0.05). The incidence of either kidney or pancreas acute rejection was also higher in the AA group (60% AA vs. 20% Caucasian, p=0.06). TAC levels were comparable at specific times after transplantation, although there was a trend toward higher doses of TAC in the AA group to achieve therapeutic levels. The incidences of relaparotomy (30% AA vs. 20% Caucasian) and major infection (40% AA vs. 60% Caucasian) were similar between groups. Renal and pancreas allograft functions were comparable between groups at specific times after transplantation. u2028Conclusions. These results suggest that SKPT in AA recipients may be associated with a higher incidence of rejection and immunologic graft loss compared to matched Caucasian controls.


Dialysis & Transplantation | 1996

Kidney/Bone Marrow Transplantation.

Ron Shapiro; Abdul S. Rao; Paulo Fontes; A. Zeevi; Mark L. Jordan; Velma P. Scantlebury; Carlos Vivas; H. Albin Gritsch; Robert J. Corry; M. Francesca Egidi; Maria T. Rugeles; H. L. R. Rilo; Abdelouahab Aitouche; A. J. Demetris; G. Rosner; Massimo Trucco; Witold Rybka; William Irish; John J. Fung; Thomas E. Starzl


Transplantation | 2000

RELATIONSHIP OF HISTOLOGICAL AND CLINICAL FEATURES OF FIRST ACUTE REJECTION ON RECURRENT REJECTION AND PANCREAS FAILURE.: Abstract# 1140

Lillian W. Gaber; Agnes Lo; M. Francesca Egidi; Robert J. Stratta; M. Hosein Shokouh Amiri; Hani P. Grewal; Tarik Kizilisik; Rita R. Alloway; A. Osama Gaber


Transplantation | 2000

REDEFINING THE IMPACT OF SYSTEMIC LUPUS ERYTHEMATOSUS ON RENAL ALLOGRAFTS: THE NEED FOR AGGRESSIVE SURVEILLANCE.: Abstract# 804 Poster Board #-Session: P61-III

M. Francesca Egidi; Naseeruddin A. Khan; Karen L. Hardinger; Lillian W. Gaber; Robert J. Stratta; Jennifer Trofe; Rita R. Alloway; A. Osama Gaber


Transplantation | 2000

EVOLVING EXPERIENCE OF HBV PROPHYLAXIS IN LIVER TRANSPLANT RECIPIENTS.: Abstract# 779 Poster Board #-Session: P36-III

Marsha R. Honaker; M. Hosein Shokkouh-Amiri; Rita R. Alloway; Hani P. Grewal; Karen L. Hardinger; Tarik Kizilisik; Trine N. Bagous; Jennifer Trofe; Santiago R. Vera; Robert J. Stratta; M. Francesca Egidi; A. Osama Gaber


Transplantation | 2000

A LOW DOSE, SHORT COURSE OF MYCOPHENOLATE MOFETIL (MMF) IN COMBINATION WITH TACROLIMUS AFTER ADULT LIVER TRANSPLANTATION.: Abstract# 216 Poster Board #-Session: P63-I

Hosein Shokouh-Amiri; Agnes Lo; Karen L. Hardinger; Rita R. Alloway; Jennifer Trofe; Hani P. Grewal; Santiago R. Vera; Robert J. Stratta; M. Francesca Egidi; Teresa K. Anderson; Tarik Kizilisik; A. Osama Gaber


Transplantation | 2000

IMPORTANCE OF SURVEILLANCE BIOPSY MONITORING IN SOLITARY PANCREAS TRANSPLANT PATIENTS RECEIVING TACROLIMUS AND MYCOPHENOLATE MOFETIL.: Abstract# 609

Lillian W. Gaber; Robert J. Stratta; Agnes Lo; M. Francesca Egidi; Hosein Shokouh-Amiri; Hani P. Grewal; A. Osama Gaber

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A. Osama Gaber

Houston Methodist Hospital

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Robert J. Stratta

Wake Forest Baptist Medical Center

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Agnes Lo

University of Tennessee Health Science Center

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Lillian W. Gaber

University of Tennessee Health Science Center

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Jennifer Trofe

University of Cincinnati

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Ron Shapiro

University of Pittsburgh

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