Fred. Silva. Oklahoma. CIty, OK. Renal Dysfunction due to an Arteriovenous ..... gray scale imaging with a color map of blood flow. Doppler fre- quency shifts.
EDITORIAL Tomas
Berl, Editor
Denver,
William
CO
Henrich
Dallas,
DESCRIPTION
COMMITTEE
Mark
TX
Paller
Minneapolis,
OF THE NEPHROLOGY WASHINGTON
TRAINING SCHOOL
Fred Silva Oklahoma
MN
CIty,
OK
PROGRAM AT THE UNIVERSITY OF MEDICINE
OF
The nephrology training program at the University of Washington has trained more than 150 fellows over 30 yr. starling in the l9#{243}Os under Dr. Belding Scribner. Fellowship training is supervised by 14 full-lime faculty under the direction of Dr. William Couser. with research interests that range from clinical research to cell and molecular biology. The program currently has 10 fellows in various stages of clinical and research training. The clinical training program accepts four fellows each year. The program selects the best candidates available and may accept individuals interested only in clinical training as well as candidates who seek advanced training In clinical or basic research in preparation for academic careers. Clinical fellows spend 3 months each on the renal consult services at the University of Washington Medical Center, and the Seathe VA Hospital. and Harborview Medical Center and on the kidney and kidney-pancreas transplant services at the universily. Addilionai exposure is provided to chronic hemodialysis and peritoneal dialysis at the Northwest Kidney Center, bone marrow transplant paflents at the Fred Hutchinson Cancer Pesearch Center. and pediatric nephrology at Children’s Hospital Medical Center. Weekly didactic teaching
conferences
conferences.
consist
of clinical
as well as a Visiting
case
Professor
discussions,
program.
Fellows
journal
clubs,
attend
clinic
renal
biopsy
conferences.
one half-day
each
and
research
week.
Pesearch activities Include immunologic and other glomerular diseases, diabetic nephropathy, hypertension, metabolic bone disease, acute renal failure, transplantation, and dialysis therapy. Fellows choosing to pursue basic research training generally enter a 3-yr training program that includes experience in both applied nephrology science under the direction of a nephrology faculty member and basic science training under the direction of selected faculty members in the basic sciences. Basic research training is supported by NIH training grants in nephrology and in molecular medicine. The University of Washington has also been designated a George M. O’Brien Kidney Pesearch Center by the NIH. Fellows choosing to pursue clinical research training enter a structured training program conducted jointly by the DMsion of Nephrology and the School of Public Health designed to prepare individuals for an academic career focused on clinical research.
Renal Dysfunction due to an Arteriovenous Transplant Recipient1 Karen
L. Harrison,
Hanh
V. Nghiem,
Douglas
M. CoIdweII,
and
Fistula in a
Connie
1. Davis2
remain
asymptomatic
K.L,
tension,
and/or
raphy;
however,
H,V. Nghiem, ogy, Universily Seattle, WA
sive and nonnephrotoxic, has become tool In the localization of a postblopsy postbiopsy AVF are asymptomatic and neously. Conversely, AVF may enlarge symptomatic, requiring embolizatlon
Harrison. CL. Davis, Department of Medicine, Division of Nephrology and Division of Transplantation, Universily of Washington School of Medicine, Seattle, WA
(J. Am.
Soc.
Nephrol.
ABSTRACT Arteriovenous renal biopsy 1 Poc&ved
D.M. Coldwell, of Washington
Transplantation
17. 1993. ACcepted to Dr. C.L
Services,
1959
Davis,
March
Un!vorslly
NE Pacific,
P043,
Copyright
1300
percutaneous Flstulae may
10, 1994.
of the American Soctely of Nephrology C by the Arner$can Society of Nephrology
Seattle,
to hematuria,
insufficiency. of an AVF has traditionally been
hyper-
The Identification made with anglog-
ulfrasonography,
which
is less invaa valuable fistula. Most close sponta-
and to
become reverse
or
prevent a renal
ol Washington
1046.6673/0506.01300$03OO/O
Journal
of RadiolMedicine,
of
5:1300-1306)
flstulae (AVF) occur after In up to 1 8% of patients.
September
2 Correspondence
1994;
Department School
or lead
renal
Medical
WA 98195.
Center.
complications. A case of renal Insufficiency In transplant recipient due to a postbiopsy AVF is presented. Spontaneous closure of the AVF resulted in the resolution of renal insufficiency. One must suspect an AVF when renal insufficiency occurs in an allograft after biopsy. Further study is needed to identify ulfrasound characteristics tory of postbiopsy Key Words:
Postbiopsy,
that
will
predIct
the
natural
his-
AVF. complication,
color
flow
Doppler
ultrasound
Volume
5
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1994
#{149}
Harrison
A
rteriovenous
fistulae
(AVF)
are
uncommon of percutaneous Most AVF are regress: howhematuria, and an
but well-known complication native and transplant renal biopsy. asymptomatic and often spontaneously ever, AVF may result in hypertension, renal insufficiency ( 1- 1 3). We present renal transplant recipient who developed
a
cadaveric
insufas demonstrated by color flow Doppler ultrasound. Three days later, the serum creatinine had returned to baseline and angiography showed resolution of the fistula. The differential diagnosIs of posttransplant renal dysfimction should include AVF, in addition to cycbosporine toxicity. rejection, obstruction, and recurrent or cle novo renal disease. ficiency
secondary
CASE
to a large,
renal
postbiopsy
AVF
REPORT
A 27-year-old white woman developed end-stage renal failure as a result of chronic pyebonephrltis secondary to ureteral reflux. She received a six-antigen-matched living donor kidney from her mother in May 1990 that failed in June 1992 secondary to antineutrophil
cytoplasmic
antibodies
(ANCA)-nega-
tive, antiglomerular basement membrane-negative crescentic glomerular nephritis. Hemodialysis was instituted and continued until March 1993, when she received a cadaveric renal transplant. Because of prolonged donor cardiopulmonary resuscitation, the graft was biopsied after procurement with a 14-gauge Trucut needle. No pathologic abnormalities were found, and the kidney was transplanted into the patient’s left iliac fossa. Immunosuppression consisted of induction OKT3, azathioprine, and prednisone. The immediate postoperative Tc-99m MAG-3 renal scan was consistent with acute preservation injury and demonstrated
slightly
decreased
activity
at
the
lower
pole
without evidence of obstruction or urine leak. Color flow Doppler ultrasound performed 1 and 3 days posttransplantation demonstrated arterial flow to all regions of the graft. Subsequently, renal function improved and cycbosporine was initiated on postoperative day 10. The serum creatinine continued to fall, reaching 21, with
a nadir a morning
186
ng/mL
and
furosemide.
and
of
1 .8
mg/dL
on
postoperative
day
12-h trough cyclosporine level of a normal blood pressure on isradipine Seven days later, she was noted to blood pressure, an increased creati-
have an elevated nine of 2.5 mg/dL, and a cycbosporine trough level of 39 1 ng/mL. She denied fever, myalgias, change in urine output, or alteration In medication schedule. Her physical examination was significant for hypertension without orthostatic changes and the absence of allograft tenderness or bruit. Peripheral extremity edema, noted the previous week, had improved. Unnalysis demonstrated no pyuria, hematuria, or proteinunia. Color flow and pulsed Doppler ultrasound of the allograft revealed a focal (3-cm) hypoechoic lesion in
the
Doppler
Journal
lower
pole
that
waveform
of the American
had
the
characteristic
Society
color
flow
of an
of Nephrology
pattern AVF with
and re-
et al
duced perfusion to the remainder of the allograft parenchyma (Figure 1). Because of renal insufficiency and large AVF size, angiographic embollzation was recommended. The patient, however, declined intervention until the following week, and she was discharged on a reduced dose ofcyclosponine. Three days later, intra-artenial digital subtraction angiography revealed
normal
allograft
vascularity
without
evidence
of an AVF (Figure 2). Repeat color flow Doppler ultrasound showed resolution of the previous abnormalities, indicating spontaneous closure of the AVF. Concurrently, the serum creatinine had returned to 1.9 mg/dL, whereas the trough cyclosponine level remained elevated at 398 ng/mL despite a lowered dose. Ultrasound examinations performed 2 wk to 9 months later continued to show normal monphobogy of, and vascular flow to, all regions of the albograft (Figure 3).
DISCUSSION Complications of percutaneous needle biopsy indude gross hematunia, perirenal hematomas, aneurysms, and AVF (1-13). AVF result from simultaneous damage to the walls of an adjacent artery and vein, causing arteniallzed blood to be shunted into the low-pressure venous system (1 ,8). Clinically, AVF may be
asymptomatic
or associated
hematuria,
clot-induced
hypertension,
and
turia
associated
wIth
rarely, an
with a localized bruit, urinary tract obstruction, renal insufficiency. HemaAVF develops when Intrare-
nab vessels communicate with the collecting system (1 1 , 13). Severe hemorrhage may result In clot formation with secondary uretenal obstruction and renal insufficiency (1 1 , 13). The shunting of blood through
the fistulae and away from been postulated to cause increased unilateral renin and renal insufficiency. however, have not been cause ofdilution from the flstulae
demonstrated,
large
perhaps
blood
flow
through
who
have
flow
through
hematunia, has been
AVF
in patients
hypertension, estimated
and by
shunts
flow
to the
venous
renal
angiography,
tion, or hippuran clearance techniques 60 to 82% of the total unilateral renal Lower vascular resistance in the venous AVF
be-
the
(8,10,14).
Blood oped ciency
the renal parenchyma has renal ischemla, followed by production, hypertension, Elevated renal vein renins,
system
devel-
insuffidye
dilu-
to approach flow (2,8,9). outflow of the and
away
from
the peripheral renal arterial bed, resulting in decreased perfusion to the remaining parenchyma distal to the fistula. Perfusion to the remaining renal parenchyma has been shown to be reduced by as much as 28 to 85% (8,9, 14, 15). ThIs vascular steal phenomenon has been accompanied by decreased (51CrJEDTA clearance when compared with the contralateral kidney (9). Thus, in the setting of a single functioning kidney. a detectable decrease in renal function may occur. It can also be hypothesized that elevated cycbosponine levels may aggrevate AVF-induced renal ischemia
by compounding
Intrarenal
vasoconstnlction
and
1301
Renal Aliograft
Fistula
Figure 2. Infro-arterlal onstrates could
no evidence have
ciency
been
in our
The
a factor
contributing
incidence diagnosis
ofdiagnostic
study
AVF to be quite severe hematunia,
studied
evaluated.
was revealed 18%
Figure 1 Color flow Doppler sonography of the renal allograft. (A) Gray scale imaging demonstrates a focal (3-cm) hypoechoic lesion (markers) in the lower pale of the renal .
1302
(16).
The when
to
AVF
on
flable
insuffi-
incidence
the
the angiogram. the incidence
patients in
increased was
and
of
patients who developed or renal insufficiency
immediately after 1 1% incidence
angiography
mode
1). Traditionally,
Asymptomatic studies
is unknown
the
has been reported
low, but only hypertension,
Prospective
performed a 9
(3, 1 7).
to renal
ofpostbiopsy depends
gold standard for diagnosis Early retrospective studies
were
dem-
patient.
precise the
because timing
subfractlon digital angiography of vascular abnormality.
were
which
angiography
native
renal
of
fistula
to
between
performed
not
biopsy
formation
12
and
1 day
to
6
graft. (B) Color flow Doppler of the graft. An AVF is evident as an area of intense and mixed red and blue color paffern, suggesting high velocity and disturbed flow (arrows). Flow in the remainder of the graft Is diminished. (C) Pulsed Doppler demonstrates turbulent flow of the AVF with spectral broadening of the Doppler waveform and signals above and below the baseline.
Volume
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1994
Harrison
vide
noninvasive,
nosing
and
nonnephrotoxic
monitoring
methods
postbiopsy
for
vascular
et al
diag-
complica-
tions (6,7). Duplex ultrasound combines real-time gray scale imaging with pulsed Doppler imaging. Color flow Doppler ultrasound combines B-mode gray scale imaging with a color map of blood flow Doppler frequency shifts. On color flow ultrasound, an AVF is characterized
as
an
area
of intense,
mixed
color
pat-
tern resulting from high-velocity flow and disturbed flow within the fistula (5-7). With pulsed Doppler, the hemodynamic effect of an AVF is seen as a highvelocity, low-pulsatillty arterial waveform in the artery leading to the fistula, turbulent flow within the fistula and spectral broadening and flow signal above and below the baseline, and arterialization of the vein arising from the fistula (Figure 1) (6,7, 15). AVF have been identified by color flow imaging and duplex Doppler in 4 to 17.5% of allogralts 1 day to 6 months after
biopsy
(6, 15).
Resolution
occurs
in
approxi-
mately 64% on follow-up ultrasonography within 2 to 50 days (15). Color flow Doppler ultrasound has been shown to be more sensitive than duplex Doppber ultrasound for the diagnosis of AVF, as assessed by a comparison with intra-artenial digital subtraction angiognaphy (6). H#{252}bsch et aL found six vascular abnormalities by color Doppler after 10 1 native renal biopsies (6). Four abnormalities AVF, whereas
identified Doppler without sult.
were two
However,
if not
Doppler why the
months of 1 5
immediate
after patients
biopsy (1-4). LundstrOm without evidence of
postbiopsy
fistula 1 day to 6 wk AVF may not develop but that several days
angiogram later
(3).
immediately may
be
showed an AVF
nose postbiopsy AVF, comparing simultaneous
were ThIs
found
to have
demonstrates
at the required
that
time for
that 3 on the
the
of biopsy artenio-
venous connection to form. When angiography was repeated 6 wk to 4 yr after the diagnosis of an AVF, 33 to 90#{176}/oof fistulae had resolved (1-3). Thus, the timing of the diagnostic study influences the incidence of reported AVF fonmation and may explain the timing of the detection of the AVF in our patient, 28 days postbiopsy and 25 days after the last negative ultrasound examination. Duplex and color flow Doppler ultrasonognaphy pro-
Journal
of the
American
Society
of Nephrology
a
Doppler ultrasound the precise predictive unknown. The resolution of through clot formation. scnlbed clot formation
formation are no
have identifying
curateby
predict
Large ullary
are
to
be
not
needle
This
may
prospective
studies
angiography and color flow have not been performed. Thus, value of ultrasound diagnosis is fistulae Morton within
been ultrasound
is thought to occur and Charboneau dean AVF that subse-
color events
flow Doppler 6 days leading to thrombus
elucidated.
Presenfly,
characteristics
spontaneous
complications needle
examination.
not seen on the first two in our patient. Thus, alultrasound is a promising method by which to diag-
large-scale
quentiy resolved on repeat later (5). The precipitating
future
angiography
Duplex Doppler To date, color flow postbiopsy lesions or false-negative rethat very small AVF may searched for at the time
carefully
ultrasound AVF was
ultrasound examinations though color flow Doppler and increasingly sensitive Figure 3. Repeat color flow Doppler sonography ofthe renal allograft. (A) Color flow Doppler demonstrates normal color flow pattern to all areas of the allograft. (B) Pulsed Doppler demonstrates normal spectral waveform.
by
it is possible
go undetected of color explain
Identified
were aneurysms. only one abnormality. has accurately located a reported false-positive
fistula
there that
closure
ac-
or risk
of
(15).
size, penetration, with
lack
of radiologic and
sclerotic
guidance,
med-
blood vessels AVF formation
associated an Increase in 2). The smaller gauge needles (16 or 18 gauge) used with the automated biopsy guns and ultrasound needle guidance during biopsy have decreased AVF development after transplant and native renal biop(Table
1303
Renal Allograft
TABLE
Fistula
1 Incidence
of AVF after
.
Authors
percutaneous Type of Bioy
(Ref. No.), Yr
and Wiener (1), 1965 Ekelund and Undholm (2), 1971 Meng and Elkin (1 7), 1971 Lundstr#{244}m(3), 1972 K#{244}hler and Edgren (4), 1974 HUbsch et al. (6), 1990 Deane et al. (15), 1992 Renowden et aL (7), 1992 Abbreviations:
d. day;
patients
(pts)
underwent
TABLE
2. Risk factors
mo, month; unilateral
immed. or biateral
influencing
immediate;
biopsya
58 ptsb 48 18 140 50 101 p15 126 pts 208 wk. week;
percutaneous
biopsy.
in parentheses
Numbers
are references.
precipitate symptoms postbiin increased investIgation of vascular abnormalities (7). Asymp-
and detection tomatic flstulae have most frequently been located 0.4 to 0.8 cm from the renal surface (7). Biopsies performed on procured kidneys before transplantation, as occurred in this case, also result in increased AVF formation, perhaps because ofthe lack ofvisual guidance and deep needle penetration (16). Multiple renal biopsies into a kidney have reportedly resulted more frequently in AVF: however, the risk of fistula per biopsy pass has not necessarily been increased (6,7, 19). Patients with hypertension and nephrosclerosis are at increased risk for postbiopsy AVF formation (1-4, 12). Biopsies performed in transplanted kidneys beyond 1 yr after transplantation have also resulted in more frequent AVF formation and are less likely to close spontaneously, possibly because of cycbosporine artenlobopathy and fibrosis (13,15). Treatment options for AVF include observation, artenlal embolization, and surgical ligation (Table 3). small Doppler
has
been
reported
(< 1.8 cm), asymptomatic ultrasound examinations every 3 to 6 months because increasing the risk for symptom
1304
anglo. C
One
2d-1O mo 5d-13 mo Immed lmmed-5wk 2-7d 1-30d 1-4d 1_7dc
ofAVF
33 71 NS 67 NS NS 43 NS
Anglo
Doppler;
NS. not
stated.
for
fistula management examinations into not been performed. arterial embolization
have
30% ofthe renal malities in the
b
Fifty-eight
are
the
available
natural
his-
mass (1 1, 12, 14,20). Perfusion remainder of the kidney reverse
abnorafter
successful embolization (14). Surgical ligation should be reserved for lesions unsuccessfully embollzed or those causing massive bleeding. In summary, renal insufficiency may be caused by biopsy-induced AVF due to the shunting ofblood away from the renal parenchyma. The risk of symptomatic AVF after biopsy is more pronounced in the single transplant kidney and occurs more often If the patient is hypertensive,
needle
penetration
is deep,
or
larger
gauged
needles are used. Renal insufficiency that begins or worsens postbiopsy should be investigated by color flow Doppler in order to identify a hemodynamically significant AVF. Most clinically symptomatic AVF will be Identified by color flow Doppler. Small fistulae less than 1 .8 cm in diameter may be monitored by serial ultrasound examinations If the patient Is asymptomatic.
eter
may
Color should be repeated lesions may enlarge, development (13).
long
as
be appropriate AVF (5, 13).
Angio Angio Anglo Anglo Anglo CFD and CFD CFD
Transcatheter by a superselective technique is the treatment of choice for symptomatic fistulae in both native and transplant kidneys (1 1-13,20). A variety of embolization materials have been used in the management of AVF, including Gelfoam and stainless steel or platinum coils (11,12,14,20). The supersebective embolization technique limits the infarction of normal tissue to the area supplied by the arterial source of the fistulae. The estimated tissue loss postembolization by technitium and iodine scans or angiography has been found to be between 0 and
for
to
Spontaneous Regression (%)
Diagnostic Method
angiography; CFD. coior flow patient diagnosed at 4 mo.
tory
more frequently therefore resulting
Observation
16 15 11 11 18 4 17.5 7.2
mal guidelines because detailed
sies (18, 19). Early reports of native biopsies suggest that AVF are more likely to occur in the medulla (2,4,8,9). In allograft recipients, most symptomatic AVF have been found more than 1 .9 cm from the renal capsule. suggesting that biopsies reaching the medulla opsy,
Time to AVF Diagnosis
More definitive treatment should be considered if the fistula enlarges or becomes symptomatic with hypertension, hematunia, or renal insufficiency. This case, however, ifiustrates that even large symptomatic fistula may close spontaneously. Currently, only infor-
AVF formation0
Hypertension (2, 4, 12) Nephrosclerosis (2, 12) Fibrosis (12) Arterlolopathy (12) Cenfral or Medullary Biopsy (2, 4, 7) Larger Needle (14 gauge) (18) Lack of Ultrasound Guidance (16) a
Incidence of AVF (%)
No. of Biopsies
NatIve NatIve NatIve Native Native Transplant Transplant Transplant
Benneft
a
renal
Fistula
also the
monitored
patient
remains
more, observation has mild renal bleeding,
as
larger
be
may be insufficiency
in the
case
than
by
1.8
close
cm
in diam-
observation
asymptomatic.
as
Further-
appropriate 11 the patient or hypertension without
presented.
Volume
Enlargement
5
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1994
Harrison
TABLE 3. Suggested Clinical
management
of AVF
Presentation
RiSkb
0
Asymptomatic
1.8 cm
Asymptomatic
Enlarging
Observe with CFDC every 3 months (5) Observe with CFD each month 1. Observe each week (13)
or not resolving
2. Embollzatlon Symptomatic
1.
Hypertension Renal insufficiency Hematuria
Embollzatbon
2. Observe
(1 1-13, 20)
each
week?
Minimal Unknown,
may
enlarge/bleed
1. Unknown, hypertension. failure. bleedlng/hematuria 2. Anglogram-Induced infarction 1. Anglograrn-Induced infarction
Hematurla with obstruction
2. Ugatlon
Hemorrhage
3. Removal
3. Loss of graft
.
Options
b
Risk of foiiowlng
for management
management
C
CFD, color flow
Doppler.
of AVF
depending
on AVF size and/or
symtpoms.
plan.
or progressive symptoms, however, should lead to fistula embolization. In conclusion, we present a case of renal allogralt dysfunction secondary to an AVF that subsequently closed spontaneously. The AVF was caused by a biopsy performed at the time of procurement. Cyclosponine toxicity was unlikely as the cause of the patient’s renal dysfunction because renal function improved with further diuresis and a consistently high cyclosponine level after fistula closure. Cyclosponine toxicity,
biopsy.
AVF
however, ischemia.
may Overt
have exacerbated rejection was
AVF-induced
severity,
and
must
natural
suspect dysfunction
an
history AVF occurs
of
when after
postbiopsy
or
new
thank Amy preparation.
John
for her expert
secretarial
and
Journal
AR,
aneurysm:
Wiener SN: Intrarenal A complication
of the American
Society
assistance
arterlovenous of percutaneous
of Nephrology
5.
6.
7.
8.
9.
AiR
L, Lindholm
739-743. in
REFERENCES 1 . Bennett
4.
10.
ACKNOWLEDGMENTS The authors manuscript
3.
fistulae.
persistent biopsy.
1965:95:372-382. T: Arterlovenous fistubae following percutaneous renal biopsy. Acta Radlol 1971; 11:38-48. Lundstr#{246}m B: Intrarenal arteriovenous fistulas. Acta Radiol (Suppl) 1972:321:32-49. K#{246}hlerR, Edgren J: Angiographic abnormalities following percutaneous needle biopsy of the kidney. Acta Radlol (Diag,J 1974:15:515-527. Morton MJ, Charboneau JW: Arteniovenous fistula after biopsy of renal transplant: Detection and monitoring with color flow and duplex ultrasonography. Mayo Clin Proc 1989:64:531-534. H#{252}bsch PJS, Mostbeck G, Barton PP. et a!.: Evaluation of arteriovenous fistulas and pseudoaneurysms in renal allografts following percutaneous needle biopsy: Colorcoded Doppler sonography versus duplex Doppler sonography. J Ultrasound Med 1990:9:95-100. Renowden SA, Blethyn J, Cochlin DL: Duplex and cobour flow sonography in the diagnosis of post-biopsy arterlovenous flstulae in the transplant kidney. Clin Radlol 1992:45:233-237. Ekelund L, Gothlin J, Lindholm T, Lindstedt E, Mattsson K: Arteriovenous fistulas followIng renal biopsy with hypertension and hemodynarnic changes: Report of a case studied by dye-dilution technique. J Urol 1972; 108: 373-376. Lindg#{226}rdh G, Lindqvist B, Lundstrom B: Renal arterlovenous fistula followIng puncture biopsy: A hemodynamic and functional study in four cases. Scand J Urol Nephrol 1971:5: 18 1-189. O’Brien DP, Parrott TS, Walton KN. Lewis EL: Renal arterlovenous fistulas. Surg Gynecol Obstet 1974:139:
2. Ekelund
renal
also an unlikely cause of renal dysfunction because her renal function improved without added immunosuppressive treatment. Fistulae of this size producing renal insufficiency may have a significant risk of bleeding, and therefore, embolization should remain a possible treatment option. However, this case supports close observation, including color flow Doppler ultrasonography as another alternative. Further prospective postbiopsy investigations with noninvasive ultrasound examinalions are warranted to determine the incidence,
allograft
.
failure
a
One
(1 1-13, 20)
renal
2. Possible massive bleeding, progressive renal failure 1 Angiogram-Induced infarction 2. Bleeding/infarction
1 Embolizatlon
Symptomatic
Renal
of al
fistula renal
1 1 . Benoit G, Charpentier B, Roche A, Bellamy J, Mohamedi D, Fries D: Arteriocabyceal fistula after grafted kidney biopsy: Successful management by selective catheter embolization. Urology 1984:24:487-490. 12. Lawen JG, Van Buren CT, Lewis RM, Kahan BD: Artenlovenous fistulas after renal allograft biopsy: A serious complication in patients beyond one year. Clin Transplant 1990:4:357-369. 13. H#{252}bschP, Schurawltzki H, TraindI 0, Karnel F: Renal
1305
Renal Allograft
14. 15. 16. 17.
1306
Fistula
allograft arteriovenous fistula due to needle biopsy with late onset of symptoms-diagnosis and treatment. Nephron 1991:59:482-485. Winkler J, Neuman-Levin M, Boner G: A successful treatment of an intravenal arteniovenous fistula by percutaneous embolization. JAMA 1991:265:631-632. Deane C, Cowan N, Giles J, et at.: Arteriovenous fistulas in renal transplants: Color Doppler ultrasound observations. Urol Radiol 1992:13:211-217. Diaz-Buxo JA, Donadlo JV Jr: Complications of percutaneous renal biopsy: An analysis of 1 ,000 consecutive biopsies. Clin Nephrol 1975:4:223-227. Meng CH, Elkin M: Immediate angiographic manifesta-
18.
19. 20.
tions of latrogenic renal injury due to percutaneous needle biopsy. Radiology 1971:100:33-341. Mahoney MC, Racadlo JM, Merhar GL, First MR: Safety and efficacy of kidney transplant biopsy: Tru-cut needle vs sonographically guided biopty gun. AiR 1993:160: 325-326. Tung KT, Downes MO, O’Donnell PJ: Renal biopsy in diffuse renal disease-Experience with a 14-gauge automated biopsy gun. Clin Radiol 1992:46:111-113. Orzel JA, Coidwell DM, Eskndge JM: Superselective embolization for renal hemorrhage with a new coaxial catheter and steerable uidewire. Cardlovasc Intervent Radlol 1988; 1 1 :343-34g.
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