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The transplantation of gastrointestinal organs
GASTROENTEROLOGY
The Transplantation THOMAS
E. STARZL,
Pittsburgh
T
Transplant
he history
Institute,
began
to fill during
of Pittsburgh
grafting
ANDREAS Health
through
to the kidney.’
plant
with
laboratories
which
and thoracic the
TZAKIS,
Science
1959
The vacuum
the mid and late 1950s with
in several
models
TODO,
University
confined
development dominal
SATORU
of whole-organ
was largely
of Gastrointestinal
of canine
the
trans-
to study all of the intra-ab-
organs.
preciated
at
outset,
metabolic,
and immunologic
Although the
relationships
on its transplantation. Welch or right allograft
istence
except experiments
by azathioprine
paravertebral hepatic
artery
gutter
stored
by rerouting
the high-volume
return
of the host
inferior
portal
vein. the livers were destroyed
the nonimmunosuppressed
cava within
animals,
ple.5 As new growth origin
in
from
flow was re-
systemic
vena
by re-
liver into the
was revascularized
into
Insulin
venous the graft
a few days in
it was concluded
was solely responsible. This was an uninterpretation. After nearly 80 years of
research on the experimental procedure of Eck’s fistula (portacaval shunt), the dogma of 1955 was that the high concentration of hormones and nutrients in splanchnic venous blood had no relevance to liver structure or function or the capacity for regeneration.3 The presumed nonspecificity of splanchnic venous blood was the central strut of the seemingly impregnable flow hypothesis of portal physiology which held that “all blood is equal.” In spite of his mistake in attributing auxiliary graft destruction to rejection alone, what Welch had done
blood
protected
im-
from
of splanchnic
reve-
that
the liver
with
of first
was able to remove
sub-
that little was left for the combut it has long been
hepatotrophic factors available
in recent
or screened
auxiliary
substances
known
and enteric
years, they have
with nontransplant are direct
allograft
of
are multi-
of pancreatic
els that in one way or other the original
When
was the most easily identified
factors,
have become
been discovered
veins.
in 1963 under
a few days to a fraction
blood
so completely organ.
livers
apparent
the portal
of the recipient.2
and the portal
peting
became
to the portal
of the blood
portal
but deprived
nous inflow shrank within their original size.4
that the so-called
who described
of an extra (auxiliary)
auxiliary
organ
in 1955 by C.
and native were repeated
of
with identical
for the constituency
to the graft
Welch’s
model
was the coex-
of two livers in the same animal
conditions
in hu-
transplantation
literature
New York,
or iliac artery,
that rejection derstandable
yielded
Hepatic
to the scientific
dogs the insertion
successfully
of the secrets
of Albany,
a unique
it was the first vital
to be engrafted
search
was introduced
When
of the model
stance(s)
not only because the kidney
the aorta
an experimental
The principle
jection
the liver occupied
but also because
The
was to create
great power.
It soon
mans,
pelvis
unwittingly
access
In this revolution,
FUNG
Pennsylvania
of each of
The Liver
Stuart
JOHN
munosuppression,
the others.
position,
and Pittsburgh,
anatomic,
the intra-abdominal viscera (Figure 1) eventually influenced the conditions for transplantation of all of
beyond
Organs
delivered
it was not ap-
intimate
Center,
1993;104:673-679
mod-
descendents
(double-liver)
of
prepara-
tions.’ The liver-replacement plantation) ported
operation
in common
clinical
by Jack Cannon
who cited Welch’s
for his own
“several
article
of California, as the stimulus
successful”
replacement
survival
of the patient.“7
in dogs “without
trans-
use today was first re-
of the University
Los Angeles, tions
(orthotopic
operaWith
the assumption that the liver played an important role in rejection, Cannon speculated that the graft would not contribute
to its own
new operation
were not given,
repudiation.
Details
of his
and the procedure
re-
mained virtually unknown until major programs of canine “orthotopic” liver transplantation were begun at the Peter Bent Brigham Hospital (Harvard)’ and independently at Northwestern University in Chicago.” At the time, there was no effective way to prevent rejection, nor would this objective be achievable for several more years. 0 1993 by the American
Gastroenteroiogical 00 16-5085/93/$3.00
Association
674
STARZL
Figure
1.
The complex
The Boston Moore tutional tended initial
GASTROENTEROLOGY
ET AL.
of intra-abdominal
effort under
the direction
was part of an immunologically commitment back
a modulator
than
of insulin a new
activity
of Francis
The
D.
instithat exwith
an
that the liver was
technique
of the metabolic of total
operation),”
in-
hepatectomy and ulti-
the insertion of an allograft into the vacated fossa,” were viewed at first as tools for meta-
bolic investigations. The superior liver-supporting
qualities
of portal
ve-
nous blood were easily demonstrable by the results of the transplant experiments.” The other requirements for successful liver replacement also were straightforward. Intraportal infusion of the transplanted liver with chilled solutions during its removal allowed effective short-term storage in much the same way as in clinical operating rooms today.’ Improved infusates in the succeeding years13*14 eventually replaced the originally used lactated Ringer’s and saline solutions. Since 1987, the University of Wisconsin solution developed by Belzer and Southard15 has permitted the safe refrigeration of human livers for 18-24 hours. Orthotopic
liver
transplantation
could
not
liver-pancreas,
be ac-
intestine,
complished
consistently
nal
bypasses
venous
from
the
pools
to the superior
anhepatic
Northwestern
or in turn was governed
In the course
(the first half of a transplant
from which come
oriented
previously
from a hypothesis
b Y this hormone.” vestigations,
a decade
on the kidney.”
stemmed
(center)
to organ transplantation
more
emphasis
initiative
mately hepatic
viscera
formed
occluded
in dogs without passively
splanchnic
stage while
vena
No. 3
or liver grafts (periphery).
pancreas,
that
Vol. 104,
and
exterblood
systemic
cava during
recipient
plastic
redirected
venous
the so-called
hepatectomy
was per-
and the new liver was sewn in.8,9 Such venous
decompression most
clinical
ever,
the
introduction
passes without stressful competent
was later
shown
to be expendable
cases by experienced in 1983
anticoagulation
and placed general
surgeons.16 of pump-driven
by-
made the operation
less
it well within and vascular
in
How-
the grasp of most
surgeons.”
The sense of futility in the late 1950s at developing an operation that had no conceivable clinical use changed
abruptly
Dameshek of 6-mercaptopurine
with the discovery the
by Schwartz
immunosuppressive qualities in nontransplant models. With
and of the
demonstration by Schwartz and Dameshek and workers in other laboratories that the drug mitigated the rejection of skin and kidney allografts in rats and dogs, respectively, the stage was set for the introduction by Murray et al. of the 6-mercaptopurine analogue azathioprine for clinical renal transplantation.18 The combination of this drug with prednisone’” permitted a treatment policy to be evolved that could be used with a succession of baseline drugs - azathioprine, cyclophosphamide, cyclosporine, and FK 506 -over the
March
1993
TRANSPLANTATION
next 30 years. In these drug cocktails, verable
prednisone
modulation
allowed
on a day-to-day
phocyte
globulin
adjunct
for induction
substitute
(ALG)
for
ALGs
changes
basis.
treatment
or as a prednisone
preparations
were succeeded
laboratory
sity of Colorado, sone was shown
there.
of kidney
when
coagulopathy
operating
of
room
General
the rest of 1963 and January
attempts
were made-four
Boston
and Paris.
6’/2-23
days, pessimism
self-imposed
When
moratorium
cipal concerns did not allow
in Denver settled
1,
atresia in the
duction
ended
combined
with
prednisone
first 12 liver
recipients
worldwide
achievable.
experience, center
available immunosuppression trol rejection. By the summer at least partially laboratory
had become
research,
first long survivor a time
cancer
during
an intensive
and on July
had been period
23 the trial
was re-
girl whose
liver contained
Although
she became
The
child
died
a the
it was
of recurrent
rate never fell below
50% in cases that
liver
also recorded court
liver
graft
in a multi-
transplantation
of last appeal
liver diseases, otherwise
The principal became
and
for al-
and even for se-
nonresectable
limitation
an inadequate
hepatic
of the technol-
supply
of organs
to
needs.
Multivisceraland Intestinal Transplantation
of
after 400 days, and for the next dozen years the
1 -year mortality
with
that
15% in the Pittsburgh
By now,
the accepted
patients
ogy quickly
to con-
after liver transplantation,22
of triumph.
lected
patient
another
trial.
meet the burgeoning
of 1967, these deficiencies rectified
sumed with a 1 M-year-old nonresectable hepatoma. not
was inadequate
the
and
of FK 506 for cyclo-
l-year
an improvement
European
malignancies.
that
cyclosporine
1 year,25 and 7 are
rate of at least 70% was readily
With the substitution
enough
and
with
in
Of our
as the news was confirmed
survival
most all nonneoplastic
to be manageable,
depletion
still alive more than a dozen years later. New programs
such a complex operation, that the intraoperative medical management (including coagulation) was not well understood
treated
rate increased
of
intro-
this drug was
cocktails.24
11 lived for more than
survival
performance
use.
clinical
or lymphoid
the first of the cyclosporine-based
of
from the
its practical Calne’s
in 1979,23 when
with
of preservation
after
of cyclosporine
benefits
but always with
rate resulting
was too great to allow frustration
1968.
(Bismuth,
miraculous
that the mortality
in 1989,26 the
a
Paris
it was successful,
di-
who had
in Hannover,
and
the nearly
when
sporine
that lasted 3 years. The prin-
for the deliberate
1972)
died after
in worldwide
subsequently
1974) also reported
a 1 -year patient
and one each in
program
this operation
proliferated
1964, six more
liver
established
(Pichlmayr,
prednisone,
Hospital.
all of the patients
were that the methods time
on March
bled to death
Colorado
in
in 1962 and
a child with biliary
and an intractable
in February
a second teams
jus-
were being
opened
The
therapy
could
England,
operation
on to the liver.21
replacement
this far. The same questions
675
liver trans-
rected to Roy Calne of Cambridge,
the notation
transplantation
recipients
to move
at liver
1963, ended tragically
experi-
to the Univer-
antirejection
transplant
was made
first attempt
Through
kidney
effort that had brought
Germany
After azathioprine-predni-
to be effective
1963, a decision The
was moved
and a clinical
was started
a handful
by mono-
University
if such a small dividend
tify the prodigious
Other
such as 0KT3.
transplant
program
eventually
ORGANS
asked increasingly plantation
as a short-term
intervention2’;
In late 1961, the Northwestern mental
in immune
In 1966, antilym-
was added
secondary
these polyclonal clonal
quick
the dose-maneu-
OF GASTROINTESTINAL
At the same orthotopic ment
in Boston
University tinal
liver
time
in the summer
transplantation and Chicago,
of Minnesota
transplantation
the first of numerous
of 1958
was under Richard
began
studies
as
develop-
Lillehei
of the
of small
intes-
in dogs2’ that led 8 years later to unsuccessful
clinical
trials.28 Be-
were accrued at the rate of about one per month. The terrible losses were concentrated in the first few post-
tween failed
operative
usually with the death of the patient.2” Although improvements in immunosuppression were being made that allowed long survival after intestinal transplanta-
months.
After
this,
the life survival
curve
flattened, leaving a residual group of stable and remarkably well survivors. Thirty (18%) of the first 170 patients in the consecutive series that started March 1,
1967 and 1987, more than a dozen attempts during the operation or up to 76 days later,
1963, and ended in December 1979 lived more than a decade, and 23 of these are still alive after 13-23 years.
tion in dogs and pigs, none of these human grafts throughout the two-decade span provided significant nutritional function.
They were all treated with azathioprine (or cyclophosphamide), prednisone, and polyclonal ALG. The continuing survival of these patients was a mute testimonial for liver transplantation, but it was
This barrier was tion was recorded cadaveric intestine graft in a recipient
broken in 1987 when graft funcfor more than a half year from a that was part of a multivisceral treated with cyclosporine, predni-
676
STARZL
GASTROENTEROLOGY
ET AL.
sane,
and OKT3.30
been
developed
1959 during
cording stem
artery
organs,
operation
could
to the surgical
The grapes,
be removed objectives,
but
both
were preserved.
The
was kept intact
up to or beyond
the liver.
The first patient who survived operation under cyclosporine-based other
died
after
patients
have been treated operation
dure in which
only
2B) was described
the liver
operation
has been particularly
the short
gut syndrome
I3 (76.5%)
outflow
lymphoma,
hyperalimentation.33
of I7 patients
tion from the original
liver
Using
modified
the composite when This
the
graft
organs
impression
A
the
was less severe were
transplanted
was confirmed
in 1969 by Calne recipients
of the organs than
under
failure
from
either
(Table
in un-
making
up
found
extended
et a1.,35 who described in pig liver protection of kidney and skin grafts
began
in March
by Goulet from
et a1.36 of
a living
related
Germany. straws in the wind.
intestinal
recipients
I), where intestinal
The routine then became
with
the results
FK
506 in
have been bet-
transplantation
than
with
Eight
operation or its liver-intestine eci of 9 r p ients survive, of whom all
but one are TPN free. The expected for general
use in the near future development
release of FK 506
is certain
to stimulate
of the intestinal
transplan-
field.
When
the intestine
able and usually
is transplanted
possible
into the host portal
vein.
so for technical reasons bypass the hepatotrophic around
was
strategy
the multivisceral
variant.33
tation
transplant
immunosuppression
isolated
rapid further
individually.34
and greatly
These were isolated
ter with
even when
transplantation
segment
by Deltz of Kiel,
Pittsburgh
com-
small intestine
possible
with
from
great to justify
intestinal
the successful
of an ileal
afforded
of the liver
for this draconian
are re-
series are
that
and
in the field
transplantation,
simpler
Enthusiasm
of cadaveric
common use of such complex gasreactivated interest in an observa-
dogs that rejection
a technically
survival
FK 506,
experiments
and intestinal
proce-
et a1.32 This
in the Pittsburgh
multivisceral
liver
surgeon
to the intestine
was sufficiently
No. 3
were performed
transplantation
1989 of a cadaveric donor
alive after @/2-30 months-all but I liberated total parenteral nutrition (TPN) (Table I). The increasingly trointestinal grafts
that the protection
to fade with
with the
useful in patients developed
only
Paris
and small bowel
who
bined
experiments
as late 1991, some workers
the same donor
but
I). A variant by Grant
believed
and by the Japanese
whose
by the concomitant
needed.
successfully
(Table
tained
after prolonged
arterial
venous
using FK 506 and are alive
after as long as I5 months (Figure
ac-
the multivisceral immunosuppres-
192 days of a B-cell
full multivisceral
As recently
or
or retained
donor,
a
with
axis and
24.
the same
Naoski Kamada, in rats.
of the celiac
(Figure
from
in
as a grape cluster
structures
sion
had
dogs
on liver transplantation.31
stem consisting
mesenteric
individual
multivisceral
nonimmunosuppressed
was envisioned
central
superior
The
early research
The allograft double
in
Vol. 104,
the liver
has not
to drain However,
alone,
it is desir-
its venous the inability
outflow to do
and the consequent need to contents of intestinal blood yet caused
serious
hepatic
complications. Another
variation
of the multivisceral
operation
is
Figure 2. The multivisceral transplantation originally developed in dogs (A) and (6) a commonly used variant in which the central organs (pancreas and duodenum) are removed, leaving the liver and small bowel. These two procedures have been used successfully in humans and provided the first examples of functioning bowel allografts. Inset: Anastomosis of host portal vein into graft portal vein.
March
TRANSPLANTATION
1993
Table 1. FK 506: Transplantation of Intestine Alone or As Part of Composite Graft
dominant
TPN free Dates Intestine
5/2/90
Liver-intestine
6/7/92 7/24/90
Total
9
8
7
17
13
12
to to
Partiala -0
and
to
3
3
whole-organ ing only
2
What
1
vided of encephalitis
and need to
above
The remaining as partial
grafts underwent which
of Figure
and intestine
below
1, in which
else’s
is discarded.37
graft has been used
for the organs
remained
differ-
large in the case and
The answers
were pro-
survivors
in the world
after kid-
by the longest
removed
at upper
from
each
liver
of these
or kidney,
well as from the patient’s
the microscope
made
them
the outset.
of the jejunum
the residual
These
grafts
along
tioned
as long as 4% years.
short
the liver
who
gastrointestinal segmental
and pancreas
bowel
have
func-
Graft Acceptance
tissues.
Then,
(immunostaining
history
recipient’s
nor and recipient
by polymerase
gerprinting”)
techniques. experiments
(Figure
nodes,
staining
and
procedures after
fluores-
the tissues were examined from
cells that
the organ
donor,
Alternatively,
chain
reaction
could
(“DNA
these analyses in animals,
the
the do-
to any specimen
came from
fin-
and from
a grand design
3) that was always the same no matter
with
ing the blood
the
special
or both.
be separated
emerged
own skin, lymph
contributions
what the engrafted
to weather
recently
to see if the individual
up had come
tion, it has not been possible to comprehend, nor even to have a plausible theory about, how grafts were able the aid of immunosuppression
after
own body,
new laboratory
of transplanta-
someone
more
or sex identification
As the answers
the modern
bearing
also from
treated recipients of hearts, lungs, and intestines. The samples were taken from the transplanted organ as
under
with
cluster
patients
and
have been
so-called
and a segment
in continuity
was the fate of the
the grafts.
cence in situ hybridization),
Throughout
all
of substituted
as the kidney
to be determined
vacating
recipients,
of these
with
changes,
from
in such organs
colon).
from
similar
ranged
other
tract
that
in the spring and early summer of were ob1992 to be restudied. 38,39 Biopsy specimens
right portion
replacement
the duodenum
of the kid-
it obvious
in the number
abdominal exenteration (spleen, liver, stomach, pancreas, duodenum, proximal jejunum, and ascending
placed
Peyer’s patches,
studies
came to Pittsburgh
pancreaticohepatic
In some
made
677
ney (30 years) or liver (23 years) transplantation,
tained the stomach
organs
of the liver to small
1
propria,
Subsequent
quantitatively
leukocytes
‘Night TPN only. bGraft removed after 239 days because stop immunosuppression therapy.
in the upper
thoracic
tissue leukocytes,
8/ 12/92
shown
nodes.
ORGANS
heart.
g/7/92 10/14/91
Multivisceral
n
Alive (l/29/93)
cells in the lamina
and mesenteric ney
OF GASTROINTESTINAL
organ.
supply
Within
minutes
of any transplant,
after restormyriad
sessile
initial attack by the recipient immune system and later to merge half forgotten into the host. Study of the
but potentially migratory leukocytes that are part of the normal structure of all organs left the graft and
gastrointestinal
migrated
vided
unique
organs insights
the liver became ognized
as having
was noted kocytes within tocytes
and their
have pro-
into these processes.38
the first transplanted a composite
that the Kupffer
became
recipients organ
(chimeric)
structure.
cells and other
predominantly
In 1969, to be rec-
recipient
It
tissue leuphenotype
100 days of transplantation, whereas the hepapermanently retained their donor specificity
(Figure 3). At the time and long afterward, this transformation was assumed to be unique to the hepatic allograft. However,
22 years later, first in rat models
and then
in humans, it was realized that the same process occurred in all successfully transplanted intestines. The epithelium of the bowel remained that of the donor, whereas the lymphoid, dendritic, and other leukocytes of recipient origin quickly invaded and became the
all over the recipient,
while
cells took their place in the transplant ing the
highly
The relocated
specialized donor
donor
and recipient
similar without
parenchymal leukocytes
recipient disturbcells. learned
to live in harmony, provided they were given sufficient protection during their nesting, by immunosuppressive viewed
drugs.
In this new context,
as traffic directors,
allowing
the drugs could be movement
of the
white cells in both directions (to and from the graft) but preventing the immune destruction that is the normal purpose of this traffic. It is not known yet how the two sets of white cellsa small population of predominantly dendritic cells from the donated organ and a large one that is in essence the entire recipient immune system of the paa “truce.” This is so complete in some tient -reach cases that immunosuppression can be stopped, particu-
678
STARZL ET AL.
GASTROENTEROLOGY Vol. 104, No. 3
G
\
V
H
I
Mutual Natural lmmunosuppression
Figure 3. The phenomenon of cell migration (with repopulation and chimerism), which is postulated to be the basis of graft acceptance. Note the interaction at the site of donorrecipient mutual cell engagement. This is thought to be the first step toward donor-specific nonreactivity (tolerance) by a mechanism of peripheral clonal “silencing.”
t
HVG larly after liver transplantation other
organs.
duced
more
planted
the critical clude
easily
by the liver
because
missionary
pluripotent
stem
the explanation
marrow prove
or spleen donor,
matching
information
and then
of various those taken
for use in humans as xenografts. and mixed chimerism phenomena inability
to accurately
predict
to be
the intes-
to shape future
alstrate-
from the bone infused
organs from
to im-
from
that
an animal
5.
The cell-migration make comprehensi-
of donor-recipient the outcome
HLA
6.
of whole
organ transplantation; neither the new organ nor its new host remains the same as at the time of the matching tests.
7. 8.
Summary a period of 33 years, it has become possible to successfully transplant individual intra-abdominal viscera or combinations of these organs. The consequences have been, first, new information about the metabolic interrelations that the visceral organs have in disease or health; second, the addition of several procedures to the treatment armamentarium of gastroOver
and third,
a more profound
by which
all whole
organ
undergrafts
References
in-
liver.
this much
diseases;
of the means
of
apparently
afforded
transplanted
of a donor
ble the unexpected
are accepted.
trans-
content
was thought
cells can be purified
including
by other
cells. This
the “acceptability”
specific
standing
that
a tool with which
gies. The migratory
intestinal
leukocytes
still incomplete,
ready provides
than
with
state can be in-
of the liver’s higher
for the protection
tine by a concomitantly While
but less constantly
Such a stable biological
organs
(Rejection)
9.
10.
11.
Woodruff WMA. The transplantation of tissues and organs. Springfield, IL: Thomas, 1960: l-61 7. Welch CS. A note on transplantation of the whole liver in dogs. Transplant Bull 1955;2:54. Bollman JL. The animal with an Eck fistula. Physiol Rev 196 1;4 1:607-62 1. Stafzl TE, Marchioro TL, Rowlands DT Jr, Kirkpatrick CH, Wilson WEC, Rifkind D, Waddell WR. lmmunosuppression after experimental and clinical homotransplantation of the liver. Ann Surg 1964; 160:4 1 l-439. Starzl TE, Watanabe K, Porter KA, Putnam CW: Effects of insulin, glucagon, and insulin/glucagon infusions on liver morphology and cell division after complete portacaval shunt in dogs. Lancet 1976; 1 :B2 l-825. Francavilla A, Starr1 TE, Porter K, Scotti-Foglieni C, Michalopou10s GK, Carrieri G, Trejo J, Azzarone A, Barone M, Zeng Q. Screening for candidate hepatic growth factors by selective portal infusion after canine eck fistula. Hepatology 1991; 14:665-670. Cannon JA. Brief report. Transplant Bull 1956;3:7. Moore FD, Smith LL, Burnap TK, Dallenbach FD, Dammin GJ, Gruber UF, Shoemaker WC, Steenburg RW, Ball MR, Belko JS. One-stage homotransplantation of the liver following total hepatectomy in dogs. Transplant Bull 1959;6:103-110. Starzl TE, Kaupp HA Jr, Brock DR, Lazarus RE, Johnson RV. Reconstructive problems in canine liver homotransplantation with special reference to the postoperative role of hepatic venous flow. Surg Gynecol Obstet 1960; 111:733-743. Moore FD. Give and take. The development of tissue transplantation. Philadelphia: Saunders, Garden City, NY, Doubleday, 1964:1-182. Starzl TE. The puzzle people. Pittsburgh: University of Pittsburgh, 1992: l-364.
March
12. 13.
14.
15. 16.
1993
Starzl TE, Bernhard
TRANSPLANTATION
VM, Benvenuto
19.
20.
21.
22.
23.
24.
25.
26.
N. A new method
27.
Lillehei
RC, Goott B, Miller FA. The physiologic
ORGANS
679
response
of the
for one-stage hepatectomy in dogs. Surgery 1959;46:880-886. Wall WJ, Calne RY, Berbertson BM, Baker PG, Smith DP, Underwood J, Kostakis A, Williams R. Simple hypothermic preservation for transporting human livers long distance for transplantation. Transplantation 1977;23:2 1 O-2 16. Benichou J, Halgrimson CG, Weil R III, Koep LJ, Starzl TE. Canine and human liver preservation for 6 to 18 hours by cold infusion. Transplantation 1977;24:4?7-411. Belzer FO, Southard JH. Principles of solid-organ preservation by cold storage. Transplantation 1988;45:673-676. Starzl TE, lwatsuki S, Van Thiel DH, Gartner JC, Zitelli BJ, Malatack JJ, Schade RR, Shaw BW Jr, Hakala TR, Rosenthal JT, Porter KA. Evolution of liver transplantation. Hepatology 1982;2:614-
small bowel of the dog to ischemia including prolonged in vitro preservation of the bowel with successful replacement and survival. Ann Surg 1959; 150:543-560. 28. Lillehei RC, ldezuki Y, Feemster JA, Dietzman RH, Kelly WK, Merkel FK, Goetz FC, Lyons GW, Manax WG. Transplantation of stomach, intestine, and pancreas: experimental and clinical observations. Surgery 1967;62:72 l-74 1. World J 29. Pritchard TJ, Krrkman RL. Small bowel transplantation. Surg 1985;9:860-867. 30. Starzl TE, Rowe M, Todo S, Jaffe R, Tzakis A, Hoffman A, Esquivel C, Porter K, Venkataramanan R, Makowka L, Duquesnoy R. Transplantatron of multiple abdominal viscera. JAMA 1989;
636.
31.
17. Shaw BW Jr, Martin DJ, Marquez
18.
R, Cortes
OF GASTROINTESTINAL
JM, Kang YG, Bugbee
26:1449-1457.
AC, Iwa-
tsuki S, Griffith BP, Hardesty RL, Bahnson HT, Starzl TE. Venous bypass in clinical livertransplantation. Ann Surg 1984;200:524534. Murray JE, Menill JP, Dammin GJ, Dealy JB, Jr, Alexandre GW, Harrison JH. Kidney transplantation in modified recipients. Ann Surg 1962; 156:337-355. Starzl TE, Marchioro TL, Waddell WR. The reversal of rejection in human renal homografts with subsequent development of homograft tolerance. Surg Gynecol Obstet 1963; 117:385-395. Starzl TE, Marchioro TL, Porter KA, lwasaki Y, Cerilli GJ. The use of heterologous antilymphoid agents in canine renal and liver homotransplantation and in human renal homotransplantation. Surg Gynecol Obstet 1967; 124:30 l-3 18. Starzl TE, Marchioro TL, Von Kaulla KN, Hermann G, Brittain RS, Waddell WR. Homotransplantation of the liver in humans. Surg Gynecol Obstet 1963; 117:659-676. Starzl TE, Groth CG, Brettschneider L, Penn I, Fulginiti VA, Moon JB, Blanchard H, Martin AJ Jr, Porter KA. Orthotopic homotransplantation of the human liver. Ann Surg 1968; 168:392-4 15. Calne RY, Rolles K, White DJG, Thiru S, Evans DB, McMaster P, Dunn DC, Craddock GN, Henderson RG, Aziz S, Lewis P. Cyclosporin A initially as the only immunosuppressant in 34 recipients of cadaveric organs: 32 kidneys, 2 pancreases, and 2 livers. Lancet 1979;2: 1033- 1036. Starzl TE, Weil R Ill, lwatsuki S, Klintmalm G, Schroter GPJ, Koep U, lwaki Y, Terasaki PI, Porter KA. The use of cyclosporin A and prednisone In cadaver kidney transplantation. Surg Gynecol Obstet 1980; 15 1: 17-26. Starzl TE, Klintmalm GBG, Porter KA, lwatsuki S, Schroter GPJ. Liver transplantation with use of cyclosporin A and prednisone. N Engl J Med 198 1;305:266-269. Stand TE, Todo S, Fung J, Demetris AJ, Venkataramanan R, Jain A. FK 506 for human liver, kidney and pancreas transplantation. Lancet 1989;2: 1OOO- 1004.
32.
Starzl TE and Kaupp HA Jr. Mass homotransplantation of abdominal organs in dogs. Surg Forum 1960; 1 1:28-30. Grant D, Wall W, Mimeault R, Zhong R, Ghent C, Garcia B, Stiller C. Duff J. Successful small-bowel/liver transplantation. Lancet
1990;335:181-184. 33.
34.
Todo villa Thiel ceral
S, Tzakis AG, Abu-Elmagd K, Reyes J, Nakamura K, CasaA, Selby R, Nour BM, Wright H, Fung JJ, Demetns AJ, Van DH, Starzl TE. Intestinal transplantation in composite visgrafts or alone. Ann Surg 1992;2 16:223-234. Starzl TE, Kaupp HA Jr, Brock DR, Butz GW Jr, Linman JW. Homotransplantation of multiple visceral organs. Am J Surg
1962;103:219-229. 35.
36.
37.
38.
39.
Calne RY, Sells RA, Pena Jr, Davis DR, Millard PR, Herbertson BM, Banns RM, Davies DAL. Induction of immunological tolerance by porcine liver allografts. Nature 1969;223:472-474. Goulet 0, Revillon Y, Canioni D, Jan D, Brousse N, Sadoun E, Colomb V, Beringer A, Hubert P, De Potter S, Discher A, Mougenot JF, Cerf-Bensussan, Ricour C. Two and one-half year follow-up after isolated cadaveric small bowel transplantation in an infant. Transplant Proc 1992;24: 1224- 1225. Starzl TE, Todo S, Tzakis A, Alessiani M, Casavilla A, Abu-Elmagd K, Fung JJ. The many faces of multivisceral transplant transplantation. Surg Gynecol Obstet 199 1; 172:335-344. Starzl TE, Demetris AJ, Murase N, lldstad S, Ricordi C. Cell migration, chimerism, and graft acceptance. Lancet 1992;339: 15791582. Starzl TE, Demetris AJ, Trucco M, Murase N, Ricordi C, lldstad S. Cell migration and chimer&m after whole organ transplantation: the basis of graft acceptance. Hepatology 1993 (in press).
Address requests for reprints to: Thomas E. Starzl, M.D., Ph.D., Department of Surgery, 3601 Fifth Avenue, 5C Falk Clinic, University 15213. of Pittsburgh, Pittsburgh, Pennsylvania Aided by project grant DK 29961 from the National Institutes of Health, Bethesda, Maryland.
The Transplantation THOMAS
E. STARZL,
Pittsburgh
T
Transplant
he history
Institute,
began
to fill during
of Pittsburgh
grafting
ANDREAS Health
through
to the kidney.’
plant
with
laboratories
which
and thoracic the
TZAKIS,
Science
1959
The vacuum
the mid and late 1950s with
in several
models
TODO,
University
confined
development dominal
SATORU
of whole-organ
was largely
of Gastrointestinal
of canine
the
trans-
to study all of the intra-ab-
organs.
preciated
at
outset,
metabolic,
and immunologic
Although the
relationships
on its transplantation. Welch or right allograft
istence
except experiments
by azathioprine
paravertebral hepatic
artery
gutter
stored
by rerouting
the high-volume
return
of the host
inferior
portal
vein. the livers were destroyed
the nonimmunosuppressed
cava within
animals,
ple.5 As new growth origin
in
from
flow was re-
systemic
vena
by re-
liver into the
was revascularized
into
Insulin
venous the graft
a few days in
it was concluded
was solely responsible. This was an uninterpretation. After nearly 80 years of
research on the experimental procedure of Eck’s fistula (portacaval shunt), the dogma of 1955 was that the high concentration of hormones and nutrients in splanchnic venous blood had no relevance to liver structure or function or the capacity for regeneration.3 The presumed nonspecificity of splanchnic venous blood was the central strut of the seemingly impregnable flow hypothesis of portal physiology which held that “all blood is equal.” In spite of his mistake in attributing auxiliary graft destruction to rejection alone, what Welch had done
blood
protected
im-
from
of splanchnic
reve-
that
the liver
with
of first
was able to remove
sub-
that little was left for the combut it has long been
hepatotrophic factors available
in recent
or screened
auxiliary
substances
known
and enteric
years, they have
with nontransplant are direct
allograft
of
are multi-
of pancreatic
els that in one way or other the original
When
was the most easily identified
factors,
have become
been discovered
veins.
in 1963 under
a few days to a fraction
blood
so completely organ.
livers
apparent
the portal
of the recipient.2
and the portal
peting
became
to the portal
of the blood
portal
but deprived
nous inflow shrank within their original size.4
that the so-called
who described
of an extra (auxiliary)
auxiliary
organ
in 1955 by C.
and native were repeated
of
with identical
for the constituency
to the graft
Welch’s
model
was the coex-
of two livers in the same animal
conditions
in hu-
transplantation
literature
New York,
or iliac artery,
that rejection derstandable
yielded
Hepatic
to the scientific
dogs the insertion
successfully
of the secrets
of Albany,
a unique
it was the first vital
to be engrafted
search
was introduced
When
of the model
stance(s)
not only because the kidney
the aorta
an experimental
The principle
jection
the liver occupied
but also because
The
was to create
great power.
It soon
mans,
pelvis
unwittingly
access
In this revolution,
FUNG
Pennsylvania
of each of
The Liver
Stuart
JOHN
munosuppression,
the others.
position,
and Pittsburgh,
anatomic,
the intra-abdominal viscera (Figure 1) eventually influenced the conditions for transplantation of all of
beyond
Organs
delivered
it was not ap-
intimate
Center,
1993;104:673-679
mod-
descendents
(double-liver)
of
prepara-
tions.’ The liver-replacement plantation) ported
operation
in common
clinical
by Jack Cannon
who cited Welch’s
for his own
“several
article
of California, as the stimulus
successful”
replacement
survival
of the patient.“7
in dogs “without
trans-
use today was first re-
of the University
Los Angeles, tions
(orthotopic
operaWith
the assumption that the liver played an important role in rejection, Cannon speculated that the graft would not contribute
to its own
new operation
were not given,
repudiation.
Details
of his
and the procedure
re-
mained virtually unknown until major programs of canine “orthotopic” liver transplantation were begun at the Peter Bent Brigham Hospital (Harvard)’ and independently at Northwestern University in Chicago.” At the time, there was no effective way to prevent rejection, nor would this objective be achievable for several more years. 0 1993 by the American
Gastroenteroiogical 00 16-5085/93/$3.00
Association
674
STARZL
Figure
1.
The complex
The Boston Moore tutional tended initial
GASTROENTEROLOGY
ET AL.
of intra-abdominal
effort under
the direction
was part of an immunologically commitment back
a modulator
than
of insulin a new
activity
of Francis
The
D.
instithat exwith
an
that the liver was
technique
of the metabolic of total
operation),”
in-
hepatectomy and ulti-
the insertion of an allograft into the vacated fossa,” were viewed at first as tools for meta-
bolic investigations. The superior liver-supporting
qualities
of portal
ve-
nous blood were easily demonstrable by the results of the transplant experiments.” The other requirements for successful liver replacement also were straightforward. Intraportal infusion of the transplanted liver with chilled solutions during its removal allowed effective short-term storage in much the same way as in clinical operating rooms today.’ Improved infusates in the succeeding years13*14 eventually replaced the originally used lactated Ringer’s and saline solutions. Since 1987, the University of Wisconsin solution developed by Belzer and Southard15 has permitted the safe refrigeration of human livers for 18-24 hours. Orthotopic
liver
transplantation
could
not
liver-pancreas,
be ac-
intestine,
complished
consistently
nal
bypasses
venous
from
the
pools
to the superior
anhepatic
Northwestern
or in turn was governed
In the course
(the first half of a transplant
from which come
oriented
previously
from a hypothesis
b Y this hormone.” vestigations,
a decade
on the kidney.”
stemmed
(center)
to organ transplantation
more
emphasis
initiative
mately hepatic
viscera
formed
occluded
in dogs without passively
splanchnic
stage while
vena
No. 3
or liver grafts (periphery).
pancreas,
that
Vol. 104,
and
exterblood
systemic
cava during
recipient
plastic
redirected
venous
the so-called
hepatectomy
was per-
and the new liver was sewn in.8,9 Such venous
decompression most
clinical
ever,
the
introduction
passes without stressful competent
was later
shown
to be expendable
cases by experienced in 1983
anticoagulation
and placed general
surgeons.16 of pump-driven
by-
made the operation
less
it well within and vascular
in
How-
the grasp of most
surgeons.”
The sense of futility in the late 1950s at developing an operation that had no conceivable clinical use changed
abruptly
Dameshek of 6-mercaptopurine
with the discovery the
by Schwartz
immunosuppressive qualities in nontransplant models. With
and of the
demonstration by Schwartz and Dameshek and workers in other laboratories that the drug mitigated the rejection of skin and kidney allografts in rats and dogs, respectively, the stage was set for the introduction by Murray et al. of the 6-mercaptopurine analogue azathioprine for clinical renal transplantation.18 The combination of this drug with prednisone’” permitted a treatment policy to be evolved that could be used with a succession of baseline drugs - azathioprine, cyclophosphamide, cyclosporine, and FK 506 -over the
March
1993
TRANSPLANTATION
next 30 years. In these drug cocktails, verable
prednisone
modulation
allowed
on a day-to-day
phocyte
globulin
adjunct
for induction
substitute
(ALG)
for
ALGs
changes
basis.
treatment
or as a prednisone
preparations
were succeeded
laboratory
sity of Colorado, sone was shown
there.
of kidney
when
coagulopathy
operating
of
room
General
the rest of 1963 and January
attempts
were made-four
Boston
and Paris.
6’/2-23
days, pessimism
self-imposed
When
moratorium
cipal concerns did not allow
in Denver settled
1,
atresia in the
duction
ended
combined
with
prednisone
first 12 liver
recipients
worldwide
achievable.
experience, center
available immunosuppression trol rejection. By the summer at least partially laboratory
had become
research,
first long survivor a time
cancer
during
an intensive
and on July
had been period
23 the trial
was re-
girl whose
liver contained
Although
she became
The
child
died
a the
it was
of recurrent
rate never fell below
50% in cases that
liver
also recorded court
liver
graft
in a multi-
transplantation
of last appeal
liver diseases, otherwise
The principal became
and
for al-
and even for se-
nonresectable
limitation
an inadequate
hepatic
of the technol-
supply
of organs
to
needs.
Multivisceraland Intestinal Transplantation
of
after 400 days, and for the next dozen years the
1 -year mortality
with
that
15% in the Pittsburgh
By now,
the accepted
patients
ogy quickly
to con-
after liver transplantation,22
of triumph.
lected
patient
another
trial.
meet the burgeoning
of 1967, these deficiencies rectified
sumed with a 1 M-year-old nonresectable hepatoma. not
was inadequate
the
and
of FK 506 for cyclo-
l-year
an improvement
European
malignancies.
that
cyclosporine
1 year,25 and 7 are
rate of at least 70% was readily
With the substitution
enough
and
with
in
Of our
as the news was confirmed
survival
most all nonneoplastic
to be manageable,
depletion
still alive more than a dozen years later. New programs
such a complex operation, that the intraoperative medical management (including coagulation) was not well understood
treated
rate increased
of
intro-
this drug was
cocktails.24
11 lived for more than
survival
performance
use.
clinical
or lymphoid
the first of the cyclosporine-based
of
from the
its practical Calne’s
in 1979,23 when
with
of preservation
after
of cyclosporine
benefits
but always with
rate resulting
was too great to allow frustration
1968.
(Bismuth,
miraculous
that the mortality
in 1989,26 the
a
Paris
it was successful,
di-
who had
in Hannover,
and
the nearly
when
sporine
that lasted 3 years. The prin-
for the deliberate
1972)
died after
in worldwide
subsequently
1974) also reported
a 1 -year patient
and one each in
program
this operation
proliferated
1964, six more
liver
established
(Pichlmayr,
prednisone,
Hospital.
all of the patients
were that the methods time
on March
bled to death
Colorado
in
in 1962 and
a child with biliary
and an intractable
in February
a second teams
jus-
were being
opened
The
therapy
could
England,
operation
on to the liver.21
replacement
this far. The same questions
675
liver trans-
rected to Roy Calne of Cambridge,
the notation
transplantation
recipients
to move
at liver
1963, ended tragically
experi-
to the Univer-
antirejection
transplant
was made
first attempt
Through
kidney
effort that had brought
Germany
After azathioprine-predni-
to be effective
1963, a decision The
was moved
and a clinical
was started
a handful
by mono-
University
if such a small dividend
tify the prodigious
Other
such as 0KT3.
transplant
program
eventually
ORGANS
asked increasingly plantation
as a short-term
intervention2’;
In late 1961, the Northwestern mental
in immune
In 1966, antilym-
was added
secondary
these polyclonal clonal
quick
the dose-maneu-
OF GASTROINTESTINAL
At the same orthotopic ment
in Boston
University tinal
liver
time
in the summer
transplantation and Chicago,
of Minnesota
transplantation
the first of numerous
of 1958
was under Richard
began
studies
as
develop-
Lillehei
of the
of small
intes-
in dogs2’ that led 8 years later to unsuccessful
clinical
trials.28 Be-
were accrued at the rate of about one per month. The terrible losses were concentrated in the first few post-
tween failed
operative
usually with the death of the patient.2” Although improvements in immunosuppression were being made that allowed long survival after intestinal transplanta-
months.
After
this,
the life survival
curve
flattened, leaving a residual group of stable and remarkably well survivors. Thirty (18%) of the first 170 patients in the consecutive series that started March 1,
1967 and 1987, more than a dozen attempts during the operation or up to 76 days later,
1963, and ended in December 1979 lived more than a decade, and 23 of these are still alive after 13-23 years.
tion in dogs and pigs, none of these human grafts throughout the two-decade span provided significant nutritional function.
They were all treated with azathioprine (or cyclophosphamide), prednisone, and polyclonal ALG. The continuing survival of these patients was a mute testimonial for liver transplantation, but it was
This barrier was tion was recorded cadaveric intestine graft in a recipient
broken in 1987 when graft funcfor more than a half year from a that was part of a multivisceral treated with cyclosporine, predni-
676
STARZL
GASTROENTEROLOGY
ET AL.
sane,
and OKT3.30
been
developed
1959 during
cording stem
artery
organs,
operation
could
to the surgical
The grapes,
be removed objectives,
but
both
were preserved.
The
was kept intact
up to or beyond
the liver.
The first patient who survived operation under cyclosporine-based other
died
after
patients
have been treated operation
dure in which
only
2B) was described
the liver
operation
has been particularly
the short
gut syndrome
I3 (76.5%)
outflow
lymphoma,
hyperalimentation.33
of I7 patients
tion from the original
liver
Using
modified
the composite when This
the
graft
organs
impression
A
the
was less severe were
transplanted
was confirmed
in 1969 by Calne recipients
of the organs than
under
failure
from
either
(Table
in un-
making
up
found
extended
et a1.,35 who described in pig liver protection of kidney and skin grafts
began
in March
by Goulet from
et a1.36 of
a living
related
Germany. straws in the wind.
intestinal
recipients
I), where intestinal
The routine then became
with
the results
FK
506 in
have been bet-
transplantation
than
with
Eight
operation or its liver-intestine eci of 9 r p ients survive, of whom all
but one are TPN free. The expected for general
use in the near future development
release of FK 506
is certain
to stimulate
of the intestinal
transplan-
field.
When
the intestine
able and usually
is transplanted
possible
into the host portal
vein.
so for technical reasons bypass the hepatotrophic around
was
strategy
the multivisceral
variant.33
tation
transplant
immunosuppression
isolated
rapid further
individually.34
and greatly
These were isolated
ter with
even when
transplantation
segment
by Deltz of Kiel,
Pittsburgh
com-
small intestine
possible
with
from
great to justify
intestinal
the successful
of an ileal
afforded
of the liver
for this draconian
are re-
series are
that
and
in the field
transplantation,
simpler
Enthusiasm
of cadaveric
common use of such complex gasreactivated interest in an observa-
dogs that rejection
a technically
survival
FK 506,
experiments
and intestinal
proce-
et a1.32 This
in the Pittsburgh
multivisceral
liver
surgeon
to the intestine
was sufficiently
No. 3
were performed
transplantation
1989 of a cadaveric donor
alive after @/2-30 months-all but I liberated total parenteral nutrition (TPN) (Table I). The increasingly trointestinal grafts
that the protection
to fade with
with the
useful in patients developed
only
Paris
and small bowel
who
bined
experiments
as late 1991, some workers
the same donor
but
I). A variant by Grant
believed
and by the Japanese
whose
by the concomitant
needed.
successfully
(Table
tained
after prolonged
arterial
venous
using FK 506 and are alive
after as long as I5 months (Figure
ac-
the multivisceral immunosuppres-
192 days of a B-cell
full multivisceral
As recently
or
or retained
donor,
a
with
axis and
24.
the same
Naoski Kamada, in rats.
of the celiac
(Figure
from
in
as a grape cluster
structures
sion
had
dogs
on liver transplantation.31
stem consisting
mesenteric
individual
multivisceral
nonimmunosuppressed
was envisioned
central
superior
The
early research
The allograft double
in
Vol. 104,
the liver
has not
to drain However,
alone,
it is desir-
its venous the inability
outflow to do
and the consequent need to contents of intestinal blood yet caused
serious
hepatic
complications. Another
variation
of the multivisceral
operation
is
Figure 2. The multivisceral transplantation originally developed in dogs (A) and (6) a commonly used variant in which the central organs (pancreas and duodenum) are removed, leaving the liver and small bowel. These two procedures have been used successfully in humans and provided the first examples of functioning bowel allografts. Inset: Anastomosis of host portal vein into graft portal vein.
March
TRANSPLANTATION
1993
Table 1. FK 506: Transplantation of Intestine Alone or As Part of Composite Graft
dominant
TPN free Dates Intestine
5/2/90
Liver-intestine
6/7/92 7/24/90
Total
9
8
7
17
13
12
to to
Partiala -0
and
to
3
3
whole-organ ing only
2
What
1
vided of encephalitis
and need to
above
The remaining as partial
grafts underwent which
of Figure
and intestine
below
1, in which
else’s
is discarded.37
graft has been used
for the organs
remained
differ-
large in the case and
The answers
were pro-
survivors
in the world
after kid-
by the longest
removed
at upper
from
each
liver
of these
or kidney,
well as from the patient’s
the microscope
made
them
the outset.
of the jejunum
the residual
These
grafts
along
tioned
as long as 4% years.
short
the liver
who
gastrointestinal segmental
and pancreas
bowel
have
func-
Graft Acceptance
tissues.
Then,
(immunostaining
history
recipient’s
nor and recipient
by polymerase
gerprinting”)
techniques. experiments
(Figure
nodes,
staining
and
procedures after
fluores-
the tissues were examined from
cells that
the organ
donor,
Alternatively,
chain
reaction
could
(“DNA
these analyses in animals,
the
the do-
to any specimen
came from
fin-
and from
a grand design
3) that was always the same no matter
with
ing the blood
the
special
or both.
be separated
emerged
own skin, lymph
contributions
what the engrafted
to weather
recently
to see if the individual
up had come
tion, it has not been possible to comprehend, nor even to have a plausible theory about, how grafts were able the aid of immunosuppression
after
own body,
new laboratory
of transplanta-
someone
more
or sex identification
As the answers
the modern
bearing
also from
treated recipients of hearts, lungs, and intestines. The samples were taken from the transplanted organ as
under
with
cluster
patients
and
have been
so-called
and a segment
in continuity
was the fate of the
the grafts.
cence in situ hybridization),
Throughout
all
of substituted
as the kidney
to be determined
vacating
recipients,
of these
with
changes,
from
in such organs
colon).
from
similar
ranged
other
tract
that
in the spring and early summer of were ob1992 to be restudied. 38,39 Biopsy specimens
right portion
replacement
the duodenum
of the kid-
it obvious
in the number
abdominal exenteration (spleen, liver, stomach, pancreas, duodenum, proximal jejunum, and ascending
placed
Peyer’s patches,
studies
came to Pittsburgh
pancreaticohepatic
In some
made
677
ney (30 years) or liver (23 years) transplantation,
tained the stomach
organs
of the liver to small
1
propria,
Subsequent
quantitatively
leukocytes
‘Night TPN only. bGraft removed after 239 days because stop immunosuppression therapy.
in the upper
thoracic
tissue leukocytes,
8/ 12/92
shown
nodes.
ORGANS
heart.
g/7/92 10/14/91
Multivisceral
n
Alive (l/29/93)
cells in the lamina
and mesenteric ney
OF GASTROINTESTINAL
organ.
supply
Within
minutes
of any transplant,
after restormyriad
sessile
initial attack by the recipient immune system and later to merge half forgotten into the host. Study of the
but potentially migratory leukocytes that are part of the normal structure of all organs left the graft and
gastrointestinal
migrated
vided
unique
organs insights
the liver became ognized
as having
was noted kocytes within tocytes
and their
have pro-
into these processes.38
the first transplanted a composite
that the Kupffer
became
recipients organ
(chimeric)
structure.
cells and other
predominantly
In 1969, to be rec-
recipient
It
tissue leuphenotype
100 days of transplantation, whereas the hepapermanently retained their donor specificity
(Figure 3). At the time and long afterward, this transformation was assumed to be unique to the hepatic allograft. However,
22 years later, first in rat models
and then
in humans, it was realized that the same process occurred in all successfully transplanted intestines. The epithelium of the bowel remained that of the donor, whereas the lymphoid, dendritic, and other leukocytes of recipient origin quickly invaded and became the
all over the recipient,
while
cells took their place in the transplant ing the
highly
The relocated
specialized donor
donor
and recipient
similar without
parenchymal leukocytes
recipient disturbcells. learned
to live in harmony, provided they were given sufficient protection during their nesting, by immunosuppressive viewed
drugs.
In this new context,
as traffic directors,
allowing
the drugs could be movement
of the
white cells in both directions (to and from the graft) but preventing the immune destruction that is the normal purpose of this traffic. It is not known yet how the two sets of white cellsa small population of predominantly dendritic cells from the donated organ and a large one that is in essence the entire recipient immune system of the paa “truce.” This is so complete in some tient -reach cases that immunosuppression can be stopped, particu-
678
STARZL ET AL.
GASTROENTEROLOGY Vol. 104, No. 3
G
\
V
H
I
Mutual Natural lmmunosuppression
Figure 3. The phenomenon of cell migration (with repopulation and chimerism), which is postulated to be the basis of graft acceptance. Note the interaction at the site of donorrecipient mutual cell engagement. This is thought to be the first step toward donor-specific nonreactivity (tolerance) by a mechanism of peripheral clonal “silencing.”
t
HVG larly after liver transplantation other
organs.
duced
more
planted
the critical clude
easily
by the liver
because
missionary
pluripotent
stem
the explanation
marrow prove
or spleen donor,
matching
information
and then
of various those taken
for use in humans as xenografts. and mixed chimerism phenomena inability
to accurately
predict
to be
the intes-
to shape future
alstrate-
from the bone infused
organs from
to im-
from
that
an animal
5.
The cell-migration make comprehensi-
of donor-recipient the outcome
HLA
6.
of whole
organ transplantation; neither the new organ nor its new host remains the same as at the time of the matching tests.
7. 8.
Summary a period of 33 years, it has become possible to successfully transplant individual intra-abdominal viscera or combinations of these organs. The consequences have been, first, new information about the metabolic interrelations that the visceral organs have in disease or health; second, the addition of several procedures to the treatment armamentarium of gastroOver
and third,
a more profound
by which
all whole
organ
undergrafts
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liver.
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diseases;
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of
apparently
afforded
transplanted
of a donor
ble the unexpected
are accepted.
trans-
content
was thought
cells can be purified
including
by other
cells. This
the “acceptability”
specific
standing
that
a tool with which
gies. The migratory
intestinal
leukocytes
still incomplete,
ready provides
than
with
state can be in-
of the liver’s higher
for the protection
tine by a concomitantly While
but less constantly
Such a stable biological
organs
(Rejection)
9.
10.
11.
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Address requests for reprints to: Thomas E. Starzl, M.D., Ph.D., Department of Surgery, 3601 Fifth Avenue, 5C Falk Clinic, University 15213. of Pittsburgh, Pittsburgh, Pennsylvania Aided by project grant DK 29961 from the National Institutes of Health, Bethesda, Maryland.