Combined Simultaneous Kidney/Bone Marrow Transplantation1

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

doi:10.1097/00007890-199560120-00009

Cited by 45 publications

(21 citation statements)

References 17 publications

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“…This analysis confirms earlier reports suggesting that bone marrow augmentation in renal transplant recipients is associated with reasonable patient and graft survival, 5,6,7,9,10 and extends these findings, with 5-year actuarial patient and graft survival rates of 85% and 76%, respectively. As in previous analyses, no significant improvement was noted in graft survival, when compared with control patients not receiving bone marrow.…”

Section: Discussionsupporting

confidence: 90%

“…As in previous analyses, no significant improvement was noted in graft survival, when compared with control patients not receiving bone marrow. 6,7,10 However, there is a suggestion that bone marrow augmentation had some immunomodulatory effect, with a trend toward a progressive decrease in the incidence of chronic allograft nephropathy. This observation has also been made by the Miami group.…”

Section: Discussionmentioning

confidence: 99%

“…[1][2][3][4][5][6][7][8][9][10][11][12][13][14] In this report, we present our experience with bone marrow augmentation in renal transplantation over the past 7 years. …”

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confidence: 99%

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Kidney transplantation with bone marrow augmentation: five-year outcomes

Shapiro

Rao

Corry

et al. 2001

Transplantation Proceedings

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Bone marrow augmentation in renal transplant recipients has been performed in a small number of centers, in an attempt to augment chimerism and/or provide donor-specific immunomodulation. [1][2][3][4][5][6][7][8][9][10][11][12][13][14] In this report, we present our experience with bone marrow augmentation in renal transplantation over the past 7 years. PATIENT AND METHODSBetween December 14, 1992, and January 1, 2000, 124 kidney/bone marrow transplants were performed. There were 51 (41%) cadaveric kidney, 59 (48%) kidney/pancreas, 8 (6%) kidney/ islet, and 6 (5%) living-related kidney recipients. The mean recipient age was 40.4 ± 10.5 years. The dosage of unmodified bone marrow was 3 to 5 × 10 8 cells/kg, given either as a single infusion (n = 86; 69%), or as multiple infusions (n = 38, 31%). 15 The mean donor age was 33.0 ± 15.5 years, and the mean cold ischemia time was 17.8 ± 9.6 hours. The mean number of HLA matches and mismatches was 1.9 ± 1.3 and 3.8 ± 1.3, respectively. Eighty patients who could have undergone kidney/bone marrow transplantation but did not because of lack of bone marrow availability were studied as controls. There were 45 (56%) cadaveric kidney, 32 (40%) kidney/pancreas, 2 (3%) kidney/islet, and 1 (1%) living-related kidney recipients in the control group. This was not a randomized trial; the availability of donor bone marrow was sporadic, and the total case material accounted for only about 10% of the transplants performed during this time period. The mean recipient age was 43.8 ± 10.8 years. The mean donor age was 36.7 ± 17.3 years, and the mean cold ischemia time was 21.9 ± 10.0 hours. The mean number of HLA matches and mismatches was 2.2 ± 1.5 and 3.5 ± 1.6, respectively.Immunosuppression was with tacrolimus-based immunosuppression, as previously described. 6,16 Antibody induction was not given, nor was radiation or cytoreduction therapy.The bone marrow and control protocols were submitted to and approved by the Institutional Review Board of the University of Pittsburgh. RESULTSThe mean follow up was 36.4 ± 23.2 months. In the K/BM group, the 1-and 5-year actuarial patient survival was 98% and 85%, and the 1-and 5-year actuarial graft survival was 97% and 76%. In the control group, the 1-and 5-year actuarial patient survival was 97% and 85%, and the 1-and 5-year actuarial graft survival was 93% arid 71 % (P = NS).

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Section: Discussionsupporting

confidence: 90%

Section: Discussionmentioning

confidence: 99%

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Kidney transplantation with bone marrow augmentation: five-year outcomes

Shapiro

Rao

Corry

et al. 2001

Transplantation Proceedings

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“…The observation of Starzl et al (1,2) that multilineage microchimerism could be detected in long-surviving recipients of organ allografts, and the argument that chimerism was an essential prerequisite for tolerance induction (1,44) prompted studies to augment natural microchimerism in an effort to promote tolerance induction in humans and reduce or eliminate dependence on immunosuppressive therapy. Recent efforts to enhance natural microchimerism in clinical organ transplantation have centered on the infusion of unmodified donor BM cells, usually at the time of transplantation (16,45,46). In principle, an alternative/additional approach is the use of specific growth factors to promote hemopoiesis, as in BM transplantation (47).…”

Section: Discussionmentioning

confidence: 99%

Microchimerism, Donor Dendritic Cells, and Alloimmune Reactivity in Recipients of Flt3 Ligand-Mobilized Hemopoietic Cells: Modulation by Tacrolimus

Morelli

Antonysamy²,

Takayama³

et al. 2000

The Journal of Immunology

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Flt3 ligand (FL) is a potent hemopoietic growth factor that strikingly enhances stem cells and dendritic cells (DC) in vivo. We examined the impact of infusing FL-mobilized bone marrow (BM) cells on microchimerism and anti-donor reactivity in normal and tacrolimus-immunosuppressed, noncytoablated allogeneic recipients. BM from B10 (H2b) mice given FL (10 μg/day; days 0–8; FL-BM) contained a 7-fold higher incidence of potentially tolerogenic immature CD11c+ DC (CD40low, CD80low, CD86low, MHC IIlow) that induced alloantigen-specific T cell hyporesponsiveness in vitro. C3H (H2k) mice received 50 × 106 normal or FL-BM cells (day 0) and tacrolimus (2 mg/kg/day; days 0–12). On day 15, enhanced numbers of donor (IAb+) cells were detected in the thymi and spleens of FL-BM recipients. Tacrolimus markedly enhanced microchimerism, which declined as a function of time. Ex vivo splenocyte proliferative and CTL responses and Th1 cytokine (IFN-γ) production in response to donor alloantigens were augmented by FL-BM infusion, but reduced by tacrolimus. Systemic infusion of purified FL-BM immature DC, equivalent in number to that in corresponding whole BM, confirmed their capacity to sensitize, rather than tolerize, recipient T cells in vivo. In vitro, tacrolimus suppressed GM-CSF-stimulated growth of myeloid DC from normal BM much more effectively than from FL-BM without affecting MHC class II or costimulatory molecule expression. Infusion of normal B10 BM cells at the time of transplant prolonged C3H heart allograft survival, whereas FL-BM cells did not. A therapeutic effect of tacrolimus on graft survival was observed in combination with normal, but not FL-BM cells. These findings suggest the need for alternative immunosuppressive strategies to calcineurin inhibition to enable the engraftment, survival, and immunomodulatory function of FL-enhanced, immature donor DC.

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“…Thus, bone marrow augmentation without recipient preconditioning was begun in December 1992, and has been done with all of the transplantable organs (kidney, pancreas, islets, liver, heart, lung, and intestine). [28][29][30][31][32] As with all of the other reported experiences, the logistic difficulties of bone marrow procurement have militated against a randomized trial, and in fact the only randomized trial of bone marrow augmentation is being performed in Miami, in liver recipients. 33 Between December 1992 and October 1996, 86 cases of bone marrow augmentation were accrued among the nearly 800 kidney transplantations at our center.…”

Section: The Pittsburgh Modelmentioning

confidence: 99%