Literature DB >> 12352907

Effect of living-related donor bone marrow infusion on chimerism and in vitro immunoregulatory activity in kidney transplant recipients.

Gaetano Ciancio1, George W Burke, Rolando Garcia-Morales, Kiliana Suzart, Anne Rosen, Camillo Ricordi, Norma S Kenyon, James M Mathew, Andreas G Tzakis, Violet Esquenazi, Joshua Miller.   

Abstract

BACKGROUND: In a previously reported series of donor-specific bone marrow cell (DBMC) infusions in cadaver kidney transplant recipients, there appeared to be an improvement in long-term graft survival (6 years) and fewer chronic rejections, which correlated with increasing DBMC chimerism (approximately 1.4% in the iliac crest bone marrow compartment now at 6 years). Prompted by this, we embarked on a study of DBMC infusion in living-related donor (LRD) kidney transplant recipients.
METHODS: Between November 1996 and May 2000, 47 LRD kidney transplant recipients received donor iliac crest marrow (1.8 x 10(8)+/-1.9 x 10(8) cells/kg body weight+/-SD) in a single infusion 4 days postoperatively. Either OKT3 (n=26) or daclizumab (n=21) were used for induction therapy, with maintenance tacrolimus, mycophenolate mofetil, and methylprednisolone immunosuppression. These recipients were prospectively compared with 39 noninfused LRD kidney transplants (control group), which received equivalent immunosuppression in the same time period. Clinical follow-up ranged from 19.0 months to 61.6 months (mean 33.2 months). Polymerase chain reaction-flow chimerism analysis and in vitro assays of immunoregulatory activity of chimeric cells were performed.
RESULTS: The incidence of acute rejection over this period of time was 10.6% and 10.3%, respectively (i.e., did not differ between groups). Immunosuppressive dosages were somewhat (but not statistically) lower over time in the DBMC group. Four-year actuarial patient and graft survival for the DBMC-infused group was 98% and 98%, and 98% and 95% for the control group, respectively ( =NS). DBMC infusion was well tolerated, with no increase in infectious episodes. DBMC chimerism in recipient iliac crest marrow has increased more rapidly than might be predicted from results previously seen in the cadaver group, despite four times fewer DBMC infused. DBMCs and (donor) peripheral blood mononuclear cells purified by immunobeads from recipient blood or bone marrow (recipient-derived donor cells) inhibited mixed leukocyte responses of the recipient to the donor more strongly than freshly obtained peripheral blood cells drawn from the donors or even compared with bone marrow cells aspirated from the donors in a previously reported group of experiments. Additionally, similarly purified recipient-derived recipient cells from the same chimeric recipient more strongly inhibited the same mixed leukocyte response reactions autologously than a large group of nonchimeric (autologous) bone marrow modulating cells in similar reactions.
CONCLUSIONS: These observations confirm that an immunoregulatory process appears to have been generated by DBMC infusion, encouraging a further decrease in immunosuppressive dosing using such assays in the future.

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Year:  2002        PMID: 12352907     DOI: 10.1097/00007890-200208270-00010

Source DB:  PubMed          Journal:  Transplantation        ISSN: 0041-1337            Impact factor:   4.939


  15 in total

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Journal:  Rev Diabet Stud       Date:  2010-08-10

2.  Regulatory T-cell subset analysis and profile of interleukin (IL)-10, IL-17 and interferon-gamma cytokine-producing cells in kidney allograft recipients with donor cells infusion.

Authors:  Moslem Ranjbar; Ghasem Solgi; Mousa Mohammadnia; Behrouz Nikbin; Gholamreza Pourmand; Bita Ansaripour; Aliakbar Amirzargar
Journal:  Clin Exp Nephrol       Date:  2012-08       Impact factor: 2.801

Review 3.  Microchimerism in promoting graft acceptance in clinical transplantation.

Authors:  James M Mathew; Joseph R Leventhal; Joshua Miller
Journal:  Curr Opin Organ Transplant       Date:  2011-08       Impact factor: 2.640

4.  Donor-derived peripheral mononuclear cell DNA is associated with stable kidney allograft function: a randomized controlled trial.

Authors:  Ghasem Solgi; Joannis Mytilineos; Vijayakrishna Gadi; Biswajit Paul; Gholamreza Pourmand; Abdolrasoul Mehrsai; Behrouz Nikbin; Ali Akbar Amirzargar
Journal:  Chimerism       Date:  2011 Oct-Dec

5.  A randomized pilot study of donor stem cell infusion in living-related kidney transplant recipients receiving alemtuzumab.

Authors:  Gaetano Ciancio; Junichiro Sageshima; Edip Akpinar; Jeffrey J Gaynor; Linda Chen; Alberto Zarak; Lois Hanson; Lissett Tueros; Giselle Guerra; Adela Mattiazzi; Warren Kupin; David Roth; Camillo Ricordi; George W Burke
Journal:  Transplantation       Date:  2013-11-15       Impact factor: 4.939

Review 6.  Hematopoietic stem cells and solid organ transplantation.

Authors:  Reza Elahimehr; Andrew T Scheinok; Dianne B McKay
Journal:  Transplant Rev (Orlando)       Date:  2016-08-03       Impact factor: 3.943

7.  Immune "tolerance profiles" in donor bone marrow infused kidney transplant patients using multiple ex vivo functional assays.

Authors:  James M Mathew; Gaetano Ciancio; George W Burke; Rolando O Garcia-Morales; Anne Rosen; Edward Wang; Carmen I Gomez; Bonnie B Blomberg; Laphalle Fuller; Violet Esquenazi; Camillo Ricordi; Joshua Miller
Journal:  Hum Immunol       Date:  2010-03-11       Impact factor: 2.850

8.  HLA-mismatched renal transplantation without maintenance immunosuppression.

Authors:  Tatsuo Kawai; A Benedict Cosimi; Thomas R Spitzer; Nina Tolkoff-Rubin; Manikkam Suthanthiran; Susan L Saidman; Juanita Shaffer; Frederic I Preffer; Ruchuang Ding; Vijay Sharma; Jay A Fishman; Bimalangshu Dey; Dicken S C Ko; Martin Hertl; Nelson B Goes; Waichi Wong; Winfred W Williams; Robert B Colvin; Megan Sykes; David H Sachs
Journal:  N Engl J Med       Date:  2008-01-24       Impact factor: 91.245

9.  Stable renal engraftment in a patient following successful tandem autologous/reduced-intensity conditioning allogeneic transplantation for treatment of multiple myeloma with del(17p) that developed as a post-transplantation lymphoproliferative disease following renal transplantation.

Authors:  Tomohiro Aoki; Masanobu Kasai; Yasuhiko Harada; Erina Matsubara; Takanobu Morishita; Tatsuya Suzuki; Makoto Tsujita; Norihiko Goto; Akio Katayama; Yoshihiko Watarai; Kazuharu Uchida; Masafumi Ito; Hiroo Saji; Toyonori Tsuzuki; Toshiki Uchida; Michinori Ogura
Journal:  Int J Hematol       Date:  2013-05-11       Impact factor: 2.490

10.  Intragraft Molecular Pathways Associated with Tolerance Induction in Renal Transplantation.

Authors:  Lorenzo Gallon; James M Mathew; Sai Vineela Bontha; Catherine I Dumur; Pranav Dalal; Lakshmi Nadimpalli; Daniel G Maluf; Aneesha A Shetty; Suzanne T Ildstad; Joseph R Leventhal; Valeria R Mas
Journal:  J Am Soc Nephrol       Date:  2017-11-30       Impact factor: 10.121

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