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Impact of Intensive Dosing of Mycophenolate on Pancreas Allograft Survival.

J. Fose,1 K. Rolling,1 N. Menninga,1 G. Leverson,2 M. Jorgenson,1 J. Odorico,2 R. Robert.2

1Pharmacy, UW Health, Madison, WI
2Transplant Surgery, UW Health, Madison, WI

Meeting: 2017 American Transplant Congress

Abstract number: C215

Keywords: Immunosuppression, Mycophenolate mofetil, Pancreas, Pancreas transplantation

Session Information

Session Name: Poster Session C: Pancreas and Islet (Auto and Allo) Transplantation

Session Type: Poster Session

Date: Monday, May 1, 2017

Session Time: 6:00pm-7:00pm

 Presentation Time: 6:00pm-7:00pm

Location: Hall D1

Purpose: The primary objective was to evaluate the effect of mycophenolate (MPA) dicharge (DC) dose on pancreas allograft (PTX) survival. Secondary endpoints included patient survival (PS), rejection, infection and time to initial MPA dose decrease.

Methods: Adult PTX recipients transplanted 1/1/2002-6/30/2015 were divided into cohorts based on MPA dose at DC; high dose (HD) – 1000 mg TID mycophenolate mofetil (MMF) or equivalent and standard dose (SD) – 1000 mg BID MMF or equivalent. Multivariable models were performed to adjust for presence of confounding risk factors.

Results: Demographics were matched between groups with no difference in transplant number, recipient BMI or age (Table 1). There was a disproportionate amount of males in HD group (HD 64.5% vs SD 50.3%, p=0.001). In a univariate analysis, graft survival was improved in the HD group at 1, 3 and 5 years (81.4, 76.1 and 69% vs 91.9, 84.1 and 77.4%, p=0.046). After adjustment for confounding risk factors there was a near significant difference across allograft subtypes (p=0.08). When censoring PAK/PTA, MPA dose had significant impact on graft failure in the SPK group (HR 1.6, p=0.007). PS, rejection and infection did not differ (p=0.4, 0.6, and 0.5). The HD group required more frequent and earlier dose reduction than the SD group [n=400, 80.9% vs n=120, 65.6%, p=0.0001), average 92.6 ± 69.3 vs 74.3 ± 72.5 days, p=0.01]

N=625 SD (n=183) HD (n=442)
Transplant type

PAK

PTA

SPK

25 (13.7%)

29 (15.8%)

129 (70.5%)

53 (12%)

65 (14.7%)

324 (73.3%)

p=0.8
Race

Caucasian

African American

Other

176 (96%)

6 (3.4%)

1 (0.6%)

406 (91.9%)

28 (63.3%)

8 (1.8%)

p=0.08
CMV

Recipient Status

Negative

Positive

Unknown

95 (51.9%)

86 (47%)

2 (1.1%)

266 (60.2%)

176 (39.8%)

0 (0%)

p=0.02

MPA Product

MMF

MPS

49 (26.8%)

134 (73.2%)

112 (25.3%)

330 (74.7%)

p=0.7
CNI at hospital DC

Tacrolimus

Cyclosporine

Neither

177 (96.8%)

3 (1.6%)

3 (1.6%)

432 (97.8%)

4 (0.9%)

6 (1.4%)

p=0.4
Induction

Thymoglobulin

Alemtuzumab

Basiliximab

Other

41 (22.4%)

58 (31.7%)

82 (44.8%)

1 (0.6%)

56 (12.7%)

162 (36.7%)

220 (49.8%)

4 (0.9%)

p=0.07

Conclusions: Use of HD MPA at PTX DC improved graft survival overall. In a subgroup analysis by allograft type dose had a significant impact on pancreas survival in SPK recipients.

CITATION INFORMATION: Fose J, Rolling K, Menninga N, Leverson G, Jorgenson M, Odorico J, Robert R. Impact of Intensive Dosing of Mycophenolate on Pancreas Allograft Survival. Am J Transplant. 2017;17 (suppl 3).

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To cite this abstract in AMA style:

Fose J, Rolling K, Menninga N, Leverson G, Jorgenson M, Odorico J, Robert R. Impact of Intensive Dosing of Mycophenolate on Pancreas Allograft Survival. [abstract]. Am J Transplant. 2017; 17 (suppl 3). https://atcmeetingabstracts.com/abstract/impact-of-intensive-dosing-of-mycophenolate-on-pancreas-allograft-survival/. Accessed May 17, 2025.

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