The clinical importance of non-HLA specific antibodies in kidney transplantation
Abstract
The clinical significance of human leukocyte antigen (HLA) antibodies (Abs) for hyperacute, acute
and chronic antibody-mediated rejection (AMR) of kidney allografts has been clearly demonstrated.
AMR occurs in the absence of donor-reactive HLA Abs. It is not known how common the problem of
AMR by non-HLA Abs is because of lack of suitable assays for their detection. It is believed that the
non-HLA Ab population, although heterogenic, is likely to target antigens on donor organ endothelial
cells (ECs). We have been involved in the clinical introduction of a flow cytometric (FC) crossmatch
(XM) test that permits the detection of Abs reactive with endothelial precursor cells (EPC) isolated
from donor peripheral blood. In this context the EPCs may function as surrogates for mature vascular
ECs.
The work in this thesis describes the adaptation of the EPCXM to detection of complement-fixing
HLA and non-HLA Abs using complement fragment-specific antibodies and flow cytometry,
describes the outcome of the EPCXM in relation to the conventional lymphocyte XM (LXM), degree of
HLA sensitization and transplantation outcome in patients evaluated for living donor (LD) kidney
transplantation (Tx), and assesses the long-term renal graft function in patients with a positive
EPCXM pre-transplant.
In the first paper, we investigated whether EPCs could be used for detection of complement-fixing
Abs and if complement factor and IgG deposition on co-purified T and B cells correlated to the
outcome of the T- and B-cell complement-dependent cytotoxicity (CDC) XM. Incubation of EPCs with
HLA Ab-positive serum samples resulted in deposition of complement factors C3c and C3d, but not
C1q nor C4d, on EPCs and co-purified lymphocytes. The amount of C3c deposition and IgG binding
on EPCs and T cells, but not B cells, correlated. The specificity and sensitivity for C3d deposition on
co-purified T cells vs the T CDC assay were 69% and 72%, while for B cells the sensitivity was
considerably lower. In the second paper, we show that 32% of the LD patients had IgG and/or IgMbinding
donor EPCs in their pre-Tx sera. Twenty-five percent of the patients were EPCXM IgM+. Of
the patients with negative LXM tests, 25% had EPC Abs mainly of IgM class not reactive with HLA.
There was no difference in rejection frequency or serum creatinine levels between the EPCXM positive
and negative groups, which is in contrast to earlier published results. However, the clinical protocols
used in the second paper included Ab pre-Tx treatments such as B cell depletion and Ab removal. The
pre-Tx EPCXM positive group had significantly more patients with delayed graft function. In the
manuscript we show that the difference in serum creatinine and glomerular filtration rates observed
between EPCXM positive and negative groups at three and six months post-Tx disappears hereafter
and during the four-year follow-up.
The detection of complement factors on EPCs and lymphocytes by flow cytometry allowing detection
of complement-fixing non-HLA and HLA Abs widens the diagnostic repertoire that can be offered
patients undergoing kidney transplantation and should thereby improve their clinical management.
Prospective studies with appropriate control groups are needed to establish whether pre-treatments
aiming at removing anti-EC Abs, as detected by the EPCXM pre-Tx, have a beneficial effect on shortand
long-term graft survival.
Parts of work
I. Detection of complement-fixing and non-fixing antibodies specific for
endothelial precursor cells and lymphocytes using flow cytometry. Ayeda
AlMahri, Jan Holgersson, Mats Alheim. Tissue Antigens, 2012, 80, 404–415. ::PMID::22931381 II. The outcome of the endothelial precursor cell crossmatch test in lymphocyte
crossmatch positive and negative patients evaluated for living donor kidney
transplantation. Mats Alheim, Ayeda AlMahri, Jakob Nilsson, Gunnar Tydén,
Jan Holgersson. Human Immunology, 2013, 74, 1437–1444. ::PMID::23777925 III. A pre-transplant positive endothelial precursor cell crossmatch does not imply
reduced long-term kidney graft function. Markus Gäbel, Ayeda AlMahri,
Lennart Rydberg, Jan Holgersson, Michael E. Breimer. (Manuscript).
Degree
Doctor of Philosophy (Medicine)
University
University of Gothenburg. Sahlgrenska Academy
Institution
Institute of Biomedicine. Department of Clinical Chemistry and Transfusion Medicine
Disputation
som för avläggande av medicine doktorsexamen vid Sahlgrenska akademin, Göteborgs universitet kommer att offentligen försvaras i Waldemar Sjölander, Medicinaregatan 7, kl. 13.00
Date of defence
2015-03-19
xalmay@gu.se
Date
2015-06-16Author
Ayeda, Almahri
Keywords
Transplantation
non-HLA antibody
Publication type
Doctoral thesis
ISBN
978-91-628-9312-5
Language
eng