BACKGROUND. Alemtuzumab (Campath-1H) induction with tacrolimus monotherapy has been shown to provide effective immunosuppression for kidney, liver, lung, and small bowel transplantation. This drug combination was evaluated in pancreas transplant recipients. METHODS. Sixty consecutive pancreas transplants (30 simultaneous pancreas-kidney, 20 pancreas after kidney, and 10 pancreas alone) were carried out under this protocol between July 2003 to January 2005. The mean follow-up was 22 months (range 17-33). RESULTS. One-year patient, pancreas, and kidney allograft survival were 95%, 93%, and 90%, respectively. With 22 months follow-up, patient, pancreas, and kidney survival were 94%, 89%, and 87%, respectively. The rejection rate was 30% (18/60), with four patients (7%) experiencing steroid-resistant rejection. Major infection occurred in three (5%) patients resulting in two (3.3%) deaths from disseminated histoplasmosis and a herpes virus infection. One patient with cryptococcal meningitis was successfully treated. Seven (11.7%) patients experienced cytomegalovirus infection, all of whom responded to treatment with ganciclovir. One (1.7%) case of polymorphic posttransplant lymphoproliferative disease was seen, which regressed with a temporary discontinuation of tacrolimus and high-dose ganciclovir. The mean serum creatinine of the 30 simultaneous pancreas-kidney transplants at one year posttransplant was 1.37±0.33 mg/ml. The preexisting creatinine in pancreas after kidney transplants was not adversely affected by this immunosuppressive protocol. CONCLUSION. A single dose of perioperative alemtuzumab followed by daily tacrolimus monotherapy provides effective immunosuppression for pancreas transplantation, but the optimal use of this drug combination is not yet clear. © 2006 Lippincott Williams & Wilkins, Inc

Abu-Elmagd

Akhtar Khan

Amadeo Marcos

Amit Basu

Calne

Ciano

Deanna Blisard

Flechner

Gruessner

Hale

Henkie P. Tan

John J. Fung

Kaufmann

Kirk

Knechtle

Kusum Tom

Marcos

McCurry

Ngoc L. Thai

Ron Shapiro

Shapiro

Starzl

Stuart

Thai

Thomas E. Starzl

Tryphonopoulos

Tzakis

Watson

English

PubMed

Thai, NL

Khan, A

Tom, K

Blisard, D

Basu, A

Tan, HP

Marcos, A

Fung, JJ

Starzl, TE

Shapiro, R

Name not available

Alemtuzumab induction and tacrolimus monotherapy in pancreas transplantation: One- and two-year outcomes

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Alemtuzumab Induction and Tacrolimus Monotherapy in Pancreas Transplantation: One- and Two-Year Outcomes

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Alemtuzumab Induction and Tacrolimus Monotherapy in Pancreas Transplantation: One- and Two-Year Outcomes Ngoc L. Thai, Akhtar Khan, Kusum Tom, Deanna Blisard, Amit Basu, Henkie P. Tan, Amadeo Marcos, John J. Fung, Thomas E. Starzl, and Ron Shapiro Background. Alemtuzumab (Campath-lH) induction with tacrolimus monotherapy has been shown to provide ef-fective immunosuppression for kidney, liver, lung, and small bowel transplantation. This drug combination was evaluated in pancreas transplant recipients. Methods. Sixty consecutive pancreas transplants (30 simultaneous pancreas-kidney, 20 pancreas after kidney, and 10 pancreas alone) were carried out under this protocol between July 2003 to January 2005. The mean follow-up was 22 months (range 17-33). Results. One-year patient, pancreas, and kidney allograft survival were 95%, 93%, and 90%, respectively. With 22 months follow-up, patient, pancreas, and kidney survival were 94%, 89%, and 87%, respectively. The rejection rate was 30% (18/60), with four patients (7%) experiencing steroid-resistant rejection. Major infection occurred in three (5%) patients resulting in two (3.3%) deaths from disseminated histoplasmosis and a herpes virus infection. One patient with cryptococcal meningitis was successfully treated. Seven (11.7%) patients experienced cytomegalovirus infection, all of whom responded to treatment with ganciclovir. One (1.7%) case of polymorphic posttransplant lymphoproliferative disease was seen, which regressed with a temporary discontinuation of tacrolimus and high-dose ganciclovir. The mean serum creatinine of the 30 simultaneous pancreas-kidney transplants at one year posttransplant was 1.37::!:O.33 mg/ml. The preexisting creatinine in pancreas after kidney transplants was not adversely affected by this immunosuppressive protocol. Conclusion. A single dose of perioperative alemtuzumab followed by daily tacrolimus monotherapy provides effective immunosuppression for pancreas transplantation, but the optimal use of this drug combination is not yet clear. Keywords: Pancreas transplantation, Immunosuppressive, Steroid-avoidance, Campath. (Transplantation 2006;82: 1621-1624) Since mid 2001, T cell depletion combined with low-dose tacrolimus mono therapy has been used as a standard pro-tocol for organ transplantation at our center (1). Lymphoid depletion with antithymocyte globulin (ATG, Thymoglobu-lin) in 2001-2002 gave way to alemtuzumab depletion from 2003 onward after it was demonstrated that alemtuzumab (Campath-IH) is a more potent agent with fewer acute side effects (2-6). However, the strategy with both antibody prep-arations was based on the same two therapeutic principles: first, reduction of global immune reactivity prior to arrival of the allograft, and second, the minimalistic use of posttrans-plant immunosuppression. The immunologic rationale be-hind the principles has been reviewed elsewhere (7, 8). The co-application of these principles with the combi-nation of alemtuzumab and tacrolimus monotherapy has been demonstrated in our center for liver (9), kidney (10,11), lung (12), and small bowel (13) transplantation. It has been possible in many of these patients to increase the interval Supported in part by the Shelly Patrick Research Fellowship. Thomas E. Starzl Transplantation Institute, University of Pittsburgh, Pitts-burgh, PA. Address correspondence to: Ngoc Thai, M.D., Ph.D., Thomas E. Starzl Transplantation Institute, UPMC Montefiore-7 South, 3459 Fifth Ave-nue, Pittsburgh, PA 15213. E-mail: thainl@upmc.edu Received 14 August 2006. Revision requested 19 September 2006. Accepted 22 September 2006. Copyright © 2006 by Lippincott Williams & Wilkins ISSN 0041-1337/06/8212-1621 001: 10. 1097/01.tp.000025071 2. 1 2389.3d Transplantation· Volume 82, Number 12, December 27,2006 between doses of maintenance tacrolimus monotherapy to every two days or even to as long one dose per week. Since both the calcineurin inhibitor drugs and prednisone are dia-betogenic, the potential attractiveness is obvious of a regimen that includes both steroid avoidance and minimum exposure to tacrolimus. However, in our previous experience with A TG-tacrolimus, the risk of rejection of pancreas grafts with the institution of space weaning was thought to be greater than that to other kinds of organ allografts (1). Consequently, in our early experience with pancreas transplantation reported here under alemtuzumab-tacrolimus, efforts were not made to space wean beyond a one dose per day for atleast one year. Moreover, wean-ing after one year was not systematically attempted. PA.TIENTS AND METHODS Immunosuppressive Protocol From July 2003 to January 2005, 60 consecutive pri-mary pancreas transplants were performed under the alemtu-zumab/tacrolimus monotherapy regimen (30 simultaneous pancreas-kidney [SPKs), 20 pancreas after kidney [PAKs], 10 pancreas alone [PTA]). Follow-up in this group of adults was to June 1,2006 with a range of 17-33 months (mean 22). The 30 mg alemtuzumab was given perioperative\y over two hours. Two grams of methylprednisolone were given, one gram as premedication for the alemtuzumab infu-sion to prevent a cytokine syndrome and the second gram at the time of pancreas allograft reperfusion. Twice-daily ta-crolimus was started orally at day one posttransplant with a 1621 ttl I 1622 12-hr trough target of 10-12 ng/ml. At one year posttrans-plant, an attempt was made in a few of the stable patients to convert to once-a-day tacrolimus with a 24-hr trough target of 7-9 ng/ml. Any further reduction oftacrolimus doses was guided by clinical status (e.g. infection, posttransplant lym-phoproliferative disease). Antibiotic prophylaxis included routine trimethoprim/ sulfamethoxasole (life-long) and nystatin (three months). Valganciclovir prophylaxis (450 mg PO daily) was main-tained for three months postoperatively for cytomegalovirus (CMV), except in the CMV seropositive donor to seronega-tive patients, where it was continued for 12 months. CMV antigenemia was performed weekly for the first three months, and monthly thereafter. Rejection was monitored by routine postoperative amy-lase and lipase levels. Elevation of these pancreatic enzymes, usually twice the baseline, would prompt an ultrasound-guided biopsy to confirm or refute allograft rejection histo-logically. Rejection scored as moderate or severe was treated with antibody therapy (usually 30 mg Campath IH). Minimal or mild acute rejection was treated with steroid boluses. No maintenance prednisone was ever added. Steroid resistance, as defined as no reduction in lipase levels after two grams of intravenous (IV) methylprednisolone for biopsy-confirmed rejection, was treated with anti-T cell antibody. In a small number of patients, mycophenolate mofetil (MMF; 500 mg twice per day) was added temporarily until amylase and lipase levels returned to baseline. However, an increase in mainte-nance tacrolimus to achieve a 12-hr trough above 10 ng/ml usually was adequate treatment. RESULTS Mortality, graft function, and other data are given sep-arately for SPK, PAK, and PTA in Table 1, and then grouped for the following overall analysis of all 60 cases. TABLE 1. Breakdown of outcomes in pancreas transplant categories SPK PAK PTA (n=30) (n=20) (n=lO) 2 2 2 year year year year year year Deaths 2 0 1 0 Patient survival (%) 97 93 100 95 90 90 Pancreas loss 3 4 0 1 1 2 Pancreas survival (%) 90 87 100 95 90 80 Kidney loss 3 4 0 Kidney survival (%) 90 87 100 95 Rejection 9 (30%) 6 (30%) 3 (30%) Infection Cytomegalovirus 4 (13%) 1 (5%) 2 (20%) Cryptococcal meningitis 0 1 (5%) 0 Human herpesvirus 6 0 1 (5%) 0 Histoplasmosis 0 0 1 (10%) Posttransplant 1 (3%) 0 0 lymphoproliferative disease Transplantation· Volume 82. Number 12, December 27, 2006 Patient and Graft Survival One-year patient survival was 95%, pancreas graft sur-vival was 93%, and renal allograft was 90%. With a mean follow-up of 22::t9 months (range 17-33 months), patient survival was 94%, pancreas graft survival was 89%, and kid-ney allograft survival was 87%. Causes of Patient Death and Graft Loss The four patient deaths were due (one each) to dissemi-nated histoplasmosis (PTA, 3 months), stroke (SPK, 13 months), autoimmune hemolytic anemia (SPK, 10 months), and sepsis (P AK, 13 months). All four had functioning pancreas grafts at the time of death. The three graft losses that occurred without patient death were caused (one each) by arterial thrombosis, rejection, and a pseudoaneurysm of an extension graft that required pancreatectomy. Rejection The overall rejection rate in this cohort over the entire follow-up period was 30%, with rejection episodes occurring between 3-18 months posttransplantation. Four patients ex-perienced pancreas allograft rejection more than one year posttransplantation. Of the 18 patients with rejection, 11 were successfully treated with boluses of methylprednisolone. The remaining seven patients with severe or moderate rejec-tion (n=3) or steroid-resistant rejection (n=4) were treated with a second lymphoid depletion (usually another dose of Campath-lH). Pancreatic rejection was highly correlated with persistently low trough tacrolimus levels, consistent with our previous report that early posttransplant pancreas rejec-tion is rare if the 12-hr tacrolimus trough is ~ 10 ng/ml (14) Beyond one year, rejection was uncommon if the tacrolimus trough level was above 7 ng/m!. Infection and Posttransplant Lymphoproliferative Disease (PTLD) Severe infection was seen in three (5%) patients, result-ing in two (3.3%) deaths, one from histoplasmosis and the other from a combined CMV /herpes virus (HHV6) infection. The third patient had cryptococcal meningitis and was suc-cessfully treated with antifungal therapy. All seven (11.7%) of 60 patients in whom cytomegalovirus infection was detected by CMV antigenemia were successfully treated with either IV gancyclovir or high dose valganciclovir (900 mg orally BID). One patient developed Epstein-Barr virus (EBV)-associated polymorphic PTLD 15 months posttransplant, manifested by a small bowel bleed requiring exploration and resection. The patient responded to a temporary cessation of tacrolimus and high-dose valganciclovir. The patient is now two years posttransplantation and doing well with function-ing allografts on once daily tacrolimus. Creatinine SPK The mean serum creatinine level in the SPK group was 1.44::tO.32 mg/dl one year posttransplantation and l.37::tO.33 mg/dl at 18 months. PAK In the P AK group, the serum creatinine provided by the prior renal allografts in 20 recipients was 1.41 ::to.27 mg/dl at :(juctlon © 2006 Lippincott Williams 6- Wilkins TABLE 2. Serum creatinine from the time of pancreas transplantation (day 0) in PAX patients Day 3 6 9 12 > 18 o months months months months months N 20 20 20 Mean 1.41 1.43 1.50 SD 0.27 0.36 0048 P value vs. 0.67 0.13 dayOa a Paired two-tailed Student's t-test. 4.0 3.5 '6 3.0 C, .§. 2.5 ~ 2.0 ' '2 ~ 1.5 (,) 1.0 0.5 . 0.0 o 3 6 20 20 1.51 1048 0044 0040 0.60 0.38 9 12 >18 Months Post Transplant nGURE 1. Months posttransplant. 19 lAS 0.38 0.13 the time of pancreas transplantation. With all but one of the 20 patients and grafts surviving for 18 subsequent months, there was no significant increase in the serum creatinine (Table 2). PTA In the PTA group, the patient who died after three months from histoplasmosis was excluded. The serum creat-inines of the other nine patients are shown individually in Figure 1. The slight upward trend in most of these patients was ascribed to tacrolimus nephrotoxicity. As expected, the nephrotoxicity was most obvious in those with preexisting renal dysfunction. DISCUSSION This experience demonstrated that a single dose of ale-mtuzumab, followed by tacrolimus monotherapy, provides effective immunosuppression for pancreas transplantation. The results were consistent with the studies of alemtuzumab reported from other centers (15-22) and by us (9-12) in which alemtuzumab was combined with various baseline im-munosuppressants for different other kinds of organ trans-plantation. In addition to the one and two year patient and graft survival, the profile of infectious and other complica-tions (including the risk of PTLD) in our pancreas recipients was similar to that usually reported under conventional mul-tiple drug immunosuppression. Despite relatively high 12 and 24 hr drug trough levels, tacrolimus monotherapy used in our protocol was relatively free of nephrotoxicity. How-ever, the optimal timing and dosage of alemtuzumab and tacrolimus remain to be determined. Wilk! Thai et al. 1623 The management policy employed for the 60 recipients reported here was strongly influenced by our prior experience between July and December 2001 with 14 pancreas recipients (10 SPK, 4 PTA) in whom the lymphoid depletion was done with a single dose of 5 mg/kg ATG (Thymoglobulin) rather than with alemtuzumab (1). In these patients, tacrolimus doses were spaced after four or more months to one dose per day, every other day, or longer intervals. The "space weaning" was associated with a high rate of rejection of the kidney, pancreas, or both organs. The diagnosis and management of pancreas rejection proved to be particularly difficult. To avoid these problems, space weaning, even to the point of one dose per day, was avoided throughout the first year in the current series. With the policy of continuous twice daily tacrolimus for the first year, the alemtuzumab-depleted patients re-ported here had a zero incidence of rejection during the first three months. From this time onward, however, 30% of the recipients experienced rejection. Efforts to reduce either the doses or the dose frequencies of tacrolimus, or to withdraw MMF after MMF had been introduced to treat breakthrough rejection, were not well tolerated. It appeared that the requi-site maintenance immunosuppression for these patients was fixed at whatever level had been arbitrarily decided upon at the outset. Of interest, the late dependence on immunosup-pression may be more pronounced than that observed in the 14 ATG-depleted patients of2001 (23). The differences between the two series do not consti-tute a comparison between ATG and alemtuzumab. It has been increasingly recognized that alloengraftment/tolerance mechanisms can be subverted by the timing and quantity of posttransplant immunosuppression thereby contributing to the amount of treatment needed chronically (8, 24, 25). With this insight, better strategies for the more efficient combined use of alemtuzumab and tacrolimus should be possible (25). REFERENCES 1. Starzl TE, Murase N, Abu-Almagd K, et al. Tolerogenic immunosup-pression for organ transplantation. Lancet 2003; 361(9368): 1502. 2. Hale G, Waldmann H, Dyer M. Specificity of monoclonal antibody Campath-1. Bone Marrow Transplant 1988; 3: 237. 3. CaIne R, Friend P, Moffatt S, et al. Prope tolerance, perioperative cam-path 1 H, and low-dose cyclosporin monotherapy in renal allograft re-cipients. Lancet 1998; 351: 1701. 4. Stuart FP, Leventhal JR, Kaufman DB, et al. Alemtuzumab facilitates prednisone free immunosuppression in kidney transplant recipients with no early rejection. Am ] Transplant 2002; 2(suppI3):397. 5. Knechtle SJ, Pirsch JD, Fechner HJ Jr, et al. Campath-IH induction plus rapamycin monotherapy for renal transplantation: results of a pilot study. Am ] Transplant 2003; 3: 722. 6. Kirk AD, Hale DA, Mannon RB, et al. Results from a human renal allograft tolerance trial evaluating the humanized CD52-specific monoclonal antibody alemtuzumab (CAMPATH-IH). Transplanta-tion 2003; 76: 120. 7. Starzl TE, Zinkernagel R. Antigen localization and migration in immu-nity and tolerance. N Engl ] Med 1998; 339: 1905. 8. Starzl TE, Zinkernagel R. Transplantation tolerance from a historical perspective. NATURE Reviews: Immunology 2001; 1: 233. 9. Marcos A, Eghtesad B, Fung n, et al. Use of alemtuzumab and tacroli-mus mono therapy for cadaveric liver transplantation: with particular reference to hepatitis C virus. Transplantation 2004; 78: 966. 10. Shapiro R, Basu A, Tan H, et al. Kidney transplantation under minimal immunosuppression after pretransplant lymphoid depletion with thy-moglobulin or campath. ] Am Col/Surg 2005; 200: 505. IZ(',j mpl')(1 . i:-; pr ,I 1624 II. Shapiro R, Ellis D, Tan HP, et al. Antilymphoid antibody precondition-ing with tacrolimus mono therapy for pediatric renal transplantation. J Pediatr 2006; 148: 813. 12. McCurry K, Iacano A, Zeevi A, et al. Early outcomes in human lung trans-plantation with ThymogIobulin or Campath-IH for recipient pretreat-ment followed by posttransplant tacrolimus near-monotherapy. J Thorae Cardiovasc Surg 2005; 130: 528. 13. Abu-Elmagd K. Intestinal transplantation for short gut syndrome and gut failure: Rewarding outcomes and current consensus. Gastroenter-ology 2006; 130(2):132-137. 14. Thai NL, Abu-Almagd K, Khan A, et al. Pancreatic Transplantation at the University of Pittsburgh. Clin Transplants 2004:205. IS. Tzakis A, Kato T, Nishida S, et al. Preliminary experience with Cam-path 1 H (Cl H) in intestinal and liver transplantation. Transplantation 2003; 75: 1227. 16. Knechtle SJ, Fernandez LA, Pirsch ID, et al. Campath- I H in renal trans-plantation: The University of Wisconsin experience. Surgery 2004; 136(4):754. 17. Ciano G, Burke GW, Gaynor n, et al. A randomized trial of three renal transplant induction antibodies: early comparison of tacrolimus, myco-phenolate mofetil, and steroid dosing, and newer immune-monitoring. Transplantation 2005; 80{ 4): 457. : ,t Iji; 1rn'·-, Transplantation • Volume 82, Number 12, December 27,2006 18. Fleehner SM, Friend PI, Brockmann I, et al. Alemtuzumab induction and sirolimus plus mycophenolate mofetil maintenance for CN! and steroid-free kidney transplant immunosuppression. Am J Transplant 2005; 5: 3009. 19. Gruessner RWG, Kandaswamy R, Humar A, et al. Calcineurin inhibitor-and steroid-free immunosuppression in pancreas-kidney and solitary pancreas transplantation. Transplantation 2005; 79(9): 1184. 20. Kaufmann DB, Leventhal IR, Axelrod D, et al. A1emtuzumab induction and prednisone free maintenance immunotherapy in kidney trans-plantation: comparison with basiliximab induction - long-term re-sults. Am J Transplant 2005; 5: 2539. 21. Tryphonopoulos P, Madariaga JR, Kato T, et al. The impact of Cam-path IH induction in adult liver allotransplantation. Transplant Proe 2005; 37: 1203. 22. Watson C, Bradley IA, Friend P, et al. A1emtuzumab (CAMPATH lH) induction therapy in cadaveric kidney transplantation - efficacy and safety at five years. Am J Transplant 2005; 5: 1347. 23. Starzl TE. History of clinical transplantation. World J Surg 2000; 24: 759. 24. Starzl TE. Acquired immunologic tolerance: With particular reference to transplantation. Immunol Res 2007, in press. 25. Marcos A, Lakkis F, Starzl TE. Tolerance for organ recipients: A dash of paradigms. Liver Transplant 2006; 12: 1448. Ur:tl(H~ uf tlw: art: \ IS 

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Alemtuzumab induction and tacrolimus monotherapy in pancreas transplantation: One- and two-year outcomes

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