Score One For ‘Adult’ Stem
Cells: First Real Progress In Acute Renal Failure Therapy Shows Fast, Broad
Results
Paracrine cell signaling, not differentiation, appears to be how stem cells
work in initial phase of organ protection, repair
BETHESDA, Md. (August 16, 2005) – Acute renal failure,
or ARF, is as serious as it sounds. An estimated 40% of critical care
hospital admissions experience ARF. Estimates of their death rate range from
50% to 80%, complicated by the fact that patients with ARF often
simultaneously suffer failure of other major organ systems.
The most serious form of ARF is caused by ischemia, or
loss of blood supply to the kidneys caused by shock, blood infection or
major cardiovascular surgery, particularly in such high- risk patients as
those with diabetes, underlying renal disease, and the elderly. In the
kidneys, such “insults” lead to destruction of kidney tubular and vascular
cells, initiating a significant inflammatory response. Recovery of kidney
function that is adequate for patient survival depends primarily on the
protection and regeneration of destroyed and injured cells.
Yet virtually no progress has been made toward
development of any highly effective ARF therapy for decades. “Basically,
catastrophic loss of kidney function has remained treatment-resistant
despite dialysis and intensive care. Treating patients with ARF thus
presents a major clinical dilemma, particularly when severe ARF occurs with
multiple organ failure,” Christof Westenfelder from the University of Utah
explained. “Our laboratory has therefore been pursuing development of novel
therapeutic interventions that are urgently needed to treat this common,
devastating and costly human disease,” Westenfelder said.
Challenging the accepted theory of stem cell
operation
In a new study, Westenfelder’s team reported that
injecting stem cells similar to the type used in bone marrow transplants is
“highly renoprotective, showing almost immediate improvement in both kidney
function and degree of tissue injury, followed by accelerated regeneration
and return of function,” he said. Furthermore, “these beneficial effects are
predominantly mediated, as our data suggest, by paracrine rather than
transdifferentiation-dependent mechanisms,” the paper reported. Paracrine
indicates action instigated by nearby cells.
These new results “challenge the most popular
hypothesis of how stem cells work in kidney protection and repair, which
holds that administered stem cells enter an injured organ where they
differentiate into those cells that have been destroyed, and thus replace
them both anatomically and functionally,” Westenfelder said.
MSC paracrine effects prompt a positive cascade,
halt inflammatory response
Rather, the Utah team found that “administered stem
cells don’t stay in the kidney that has ARF long enough to differentiate
into kidney cells, but rather appear to alter the course of ARF by a number
of identifiable and some still unexplored paracrine mechanisms. The former
include the induction of organ-protective and repair-supporting genes in
surviving renal cells, robust suppression of proinflammatory cytokines in
the ARF kidney and upregulation of anti-inflammatory genes, as well as the
delivery and release at the site of injury of organ-protective and other
beneficial gene products by the stem cells per se. Collectively, these and
as yet unidentified mechanisms represent a highly potent intervention in ARF,”
Westenfelder stated.
The study, “Administered mesenchymal stem cells protect
against ischemic acute renal failure through differentiation-independent
mechanisms,” appears in the American Journal of Physiology-Renal
Physiology, published by the American Physiological Society.
Research was conducted by Florian Tögel, Zhuma Hu, Kathleen Weiss, and
Christof Westenfelder of the University of Utah and the Veterans Affairs
Medical Center; Jorge Isaac, University of Utah; and Claudia Lange, Bone
Marrow Transplantation Center, Hamburg.
Stem cell time in the kidney: about two hours
At first, Westenfelder conceded, the researchers
experienced “substantial frustration because the cells were detectable in
the kidney for only two hours and then ‘disappeared.’ But after entry into
the kidneys with ARF, we found that they fundamentally changed a number of
important gene expression profiles. In fact, the intrarenal location of
administered stem cells is such that it facilitates the delivery of
renoprotective growth factors and cytokines to the sites where kidney cells
are primarily destroyed from both the blood and urinary aspects of the cells
that must be protected and repaired!” Westenfelder reported.
With their rapid mode of action within only two hours
in the kidney, the researchers deduced that the mechanism mediating the
protective effects of MSC (mesenchymal stem cells) “must be primarily
paracrine, as implied by their demonstrated expression of several growth
factors such as HGF (hepatocyte growth factor), VEGF and IGF-1, all known to
improve renal function in ARF, mediated by their antiapoptotic, mitogenic
and other cytokine actions,” the paper said.
“Specifically, these as yet incompletely defined
paracrine actions of MSC result in the renal downregulation of
proinflammatory cytokines IL-1-beta, TNF-alpha, and IFN-gamma, as well as
iNOS (inducible nitric oxide synthase), and upregulation of
anti-inflammatory and organ-protective interleukin-10, as well as bFGF
(basic fibroblast growth factor), TGF-alpha (transforming growth factor
alpha) and antiapoptotic
Bc1-2,” the paper added.
Beneficial paracrine actions are elicited early and
late after onset of ARF
The study said it “provides the first clear evidence
that therapy with MSC affords significant renoprotection in rats with
ischemic/reperfusion (I/R) ARF. Animals infused with MSC either immediately
or 24 hours after reperfusion had significantly better renal function, lower
renal injury and cell-death scores, and higher cell division indices than
vehicle-treated control animals,” the paper stated. Indeed, administration
after 24 hours of more severe ARF had an even greater beneficial effect.
Based on utilization of several genomic and nongenomic
cell-tagging techniques, the researchers were able to follow the stem cells
as they circulated through the renal microcirculation of two different
strains of rats used in the experiments. “Although we did not detect
transdifferentiation events during the 72-hour period of observation, it is
possible that cell transdifferentiation and integration may be important at
later states of organ repair,” the study noted.
The Utah team used MSC for several reasons, notably the
fact that they can be harvested easily from bone marrow, isolated, grown in
culture and genetically engineered. To test that MSC subsequently used in
these studies retained their phenotype after being cultured, the researchers
routinely tested whether their characteristic potential to differentiate
into fat and bone cells was preserved.
The researchers conceded that it “is surprising that
the very transient presence of MSC in the injured kidney, as we document, is
sufficient to greatly ameliorate the course” of I/R ARF and also note that
the rat model of ARF used in the study is “a suitable if somewhat imperfect
model of the most common and the most treatment-resistant type of human
ischemic ARF.”
Next steps
-
Current studies are investigating the collective and
individual renoprotective capacity of cytokines temporarily released by
MSC.
-
Two clinical efforts are planned. First will be a
compassionate study in Europe next year in patients with complicated bone
marrow transplants, a setting where such stem cells already are approved
for use. If successful, a compassionate-use study in patients with severe
ARF and multiorgan failure will be designed, eventually leading to
clinical trials.
-
Though no adverse effects were seen in these experiments,
long-term studies are needed to prove that no adverse effects occur after
in vivo administration of adult MSC.
-
Also to be determined is whether renoprotective and
gene-modulating effects of MSC “are primary actions that are humorally
elicited by these cells or whether they result from the improvement of
tissue injury by as yet unknown factors released by them.”
-
Future studies “will also have to define the possible
contribution to organ protection made by the immunomodulatory effects of
MSC, as well as potential late phase contributions to organ repair via
differentiation of stem cells into cells that have been destroyed in ARF,”
the study noted.
Source and funding
The study, entitled “Administered mesenchymal stem
cells protect against ischemic acute renal failure through
differentiation-independent mechanisms,” appears in the American Journal
of Physiology-Renal Physiology, published by the American
Physiological Society. The research was conducted by Florian Tögel,
Zhuma Hu, Kathleen Weiss, and Christof Westenfelder of the Division of
Nephrology, Dept. of Medicine, University of Utah, Salt Lake City, and the
Veterans Affairs Medical Center; Tögel and Westenfelder are also at the
Dept. of Physiology; Jorge Isaac of the Dept. of Pathology; and Claudia
Lange of the Bone Marrow Transplantation Center, Hamburg, Germany.
Research was supported in part by the U.S. Dept. of
Veterans Affairs, American Heart Association, Dialysis
Research Foundation, National Kidney Foundation, Western
Institute for Biomedical Research and NHLBI (NIH).
Editor’s note: The media may obtain an
electronic version of Tögel et al. and interview members of the research
team by contacting Donna Krupa at the American Physiological Society,
(301) 634-7209, cell (703) 967-2751 or
dkrupa@the-aps.org.
* * *
The
American Physiological Society was founded in 1887 to foster basic and
applied bioscience. The Bethesda, Maryland-based society has more than
10,000 members and publishes 14 peer-reviewed journals containing almost
4,000 articles annually.
APS
provides a wide range of research, educational and career support and
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mechanisms of diseased and healthy states. In May 2004, APS received
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