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Polyarteritis Nodosa and Hepatitis B related PAN

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admitted Jan 25 to SSM -SOB, CXR bilat infiltrates, became hypertensive ... Hb 83, WBC 20, Plt 49 -no fragments, toxic vacuolation. CXR bilat lower lobe opacities ... – PowerPoint PPT presentation

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Title: Polyarteritis Nodosa and Hepatitis B related PAN

1
Polyarteritis Nodosaand Hepatitis B related PAN

Raymond Fung
Rheumatology Rounds
March 16, 2004

2
Case

41M from Sault Ste Marie
PMH
IV drug use, smoker, EtOH
known hep B hep C, HIV neg
HPI
Dec-Jan -postprandial abdominal pain and wt loss
25lbs
admitted Jan 25 to SSM -SOB, CXR bilat
infiltrates, became hypertensive
intubated, ARDS like picture, BAL neg
rx ceftazidime, levo, diflucan

3
Case - HPI

renal failure -on admission Cr. 194, then
increased to Cr 343, nonoliguric, bland urine
sediment, ? ATN
2D echo Gr 3LV, MR, RVSP 53 -Trop 2 ?myocarditis
extubated but reintubated because..
massive UGI -melena requiring gt10 PRBC
-transferred to SMH
acute transaminitis AST/ALT gt 1500, then
decreased -?shock liver
OGD -multiple large duodenal, prox jejunal ulcers

4
Case -Physical Exam

intubated, sedated
bp 110/50, HR 75
no evidence of vasculitic rash
no orchitis
heart sounds n, chest upper airway sounds
no active joints

5
Case -Lab

Hb 83, WBC 20, Plt 49 -no fragments, toxic
vacuolation
CXR bilat lower lobe opacities
Cr. 404, urine bland, heme granular casts
AST 133, ALT 75, ALP 75, TB 36
Ca 1.49, PO4 3.91, Alb 12
Trop 0.26
CK 150

6
Outline

classification and definition
epidemiology, pathology
clinical features
treatment and prognosis

7
History and classification

Kussmal and Maier 1866 -systemic vasculitis
wt loss, fever, peripheral neuropathy, renal, GI,
skin, muscle, cardiac, hypertension
1990, ACR established criteria for dx of PAN
1994 Chapel Hill Consensus conference
distinguished MPA from PAN

8
PAN -ACR criteria

wt loss gt 4kg
livedo reticularis
testicular pain/ tenderness
myalgias, weakness, tenderness
mono or polyneuropathy
diastolic bp gt 90mmHg
elevated Cr/ BUN
hep B positive
arteriogram -aneurysm or occlusion not due to
atheriosclerosis
bx PMN in small/med artery wall

9
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10
Epidemiology

annual incidence 1-9 per 1 000 000 people
affects men and women 1.1-1.9 1
all ages, peak 40-60
all racial groups
individuals at risk for HBV-PAN
older -infected via transfusion, accupuncture
unvaccinated young -IVDU, tattoo, piercing

11
Etiology

studies from early 1970s found 36 of cases
related to HBV infection
90s frequency of HBV - PAN 7, vaccination
last 2yrs, fewer than 10pts / year dx in France
HBV related PAN takes form of classic PAN
other etiologies HIV, parvovirus B19, CMV,
HTLV-1, HCV

Guillevin, L. Lhote, F. Polyarteritis nodosa
related to hepatitis B virus a prospective study
with long-term observation of 41 patients.
Medicine 1995 74(5) 238-253.
12
Pathology -blood vessels

medial fibrinoid necrosis
polymorphic panarterial cellular inflammatory
infiltrate, CD8 Tcells, macrophages, PMN
clusters plasma cells in adventitia
lesions result of immune complex deposition in
vessels
PAN -associated leukocytoclastic vasculitis of
skin

13
Sural Nerve Biopsy
14
PAN in the skin
15
Mechanism -Viral induced vasculitis

viral replication -direct injury to vessel wall
e.g equine viral arteritis
immune mediated vascular damage
circulating immune complex
formation of immune complex in situ
hepatitis B has been implicated as triggering
antigen
ANCA negative, therefore not considered part of
etiology

16
Clinical Features

majority present w consitutional symptoms
malaise, fever, wt loss
PAN usually presents within 6 months of HBV
infection
HBV-PAN presents similar to other PAN except
several manifestations more common
GI (46)
malignant hypertension (30)
renal infarction and orchitis (26)

17
Clinical -Neurologic

mononeuritis multiplex most common symptoms
motor, sensory asymmetric
predominantly affect LE
radial, cubital, median nerves less frequently
motor deficit occurs abruptly
sensory -hypo/pain in area of motor deficit
bilateral distal sensory neuropathy
CSF normal

18
Clinical Features

Other Neurologic
cranial nerve palsies rare (III, IV, VI, VII)
spinal roots, cauda equina rare
stroke, brain hemorrhage can occur
MSK
myalgies 30-70 -intense
CK usually normal
arthralgias 40
arthritis -asymmetric, larger joints lower
extremity

19
Clinical features

Skin
25-60
vascular purpura, papulopetechial
livedo reticularis
less common bullous, vesicals, SC nodules,
distal gangrene
Renal
vascular nephropathy -microaneurysms, stenoses,
infarcts
perirenal hematoma result from rupture of
aneurysms
hypertension -renin dependent

20
Cutaneous PAN

Lower extremity
tend to ulcerate
surrounding livedo

21
Cutaneous PAN
22
Cutaneous PAN

Thickened arterial wall w inflammatory infiltrate
Tunica intima -eosinophilic ring of fibrinoid
necrosis

23
Renal Aneuryms
24
Cutaneous PAN
25
Cutaneous PAN
26
Cutaneous PAN
27
Cutaneous ulcers
28
Clinical Features

GI
most severe manifestation -fatal
GI bleeding, bowel perforation
abdo pain, wt loss consequence of bowel ischemia
vasculitis of appendix, gallbladder may be first
presentation of PAN
Hep B
transaminitis usually mild-moderate
bx -may reveal chronic inflammation

29
Hepatic Aneurysms
30
SMA Aneurysm
31
Clinical Features

Cardiac
secondary to vasculitis of coronary arteries or
to severe hypertension
angina rare, angiography usually normal
Orchitis
classic symptom, more common w hep B
Retinal vasculitis

32
Back to Case

41M w hepatitis B
prodrome abdo pain/ wt loss
respiratory illness with renal failure,
hypertension, cardiac failure
profuse GI bleeding w multiple ulcers
(already 4 criteria)
Rheum requested MRA
beading of mesenteric vessels in splenic,
hepatic, and sup mesenteric arteries
tapering of renal arteries

33
Case -Clinical Course

pulse solumedrol 1g X3d Feb 14-16
Solumedrol 80mg BID
plasma-exchange Feb 16 X5d, Feb 23, Feb 25
IV IG Feb 20, 21
lamivudine started Feb 16

34
Treatment of PAN

untreated 5yr mortality gt90
corticosteroids 1950s survival 50 at 5yrs in
late 1970s
other therapies
cyclophosphamide
plasma exchanges

35
Treatment of PAN -Steroids

methylprednisolone pulses 15mg/kg 1g IV q24h
widely used for severe systemic vasculitis
life-threatening organ involvement, extension of
mononeuritis multiplex
?need such high doses
begin corticosteroids 1mg/kg/d until clinical
improvement, ESR normal
taper, usually within 1month
more rapid taper if cyclophosphamide used
stopped 9-12 months

36
Adjunctive Therapies

is cyclo necessary for the treatment of PAN?
should it be used in certain subgroups? i.e. Are
there certain prognostic factors that we can use
to choose between steroid alone vs. steroid plus
cyclo?
is plasma exchange necessary?
does adding plasma exchange to steroids make a
difference?

37
French Vasculitis Study Group

Prognostic Factors in Polyarteritis Nodosa and
Churg-Strauss Syndrome
prospective study of 342 patients
Guillevin, Loic Medicine Jan 1996
Long Term Followup of Polyarteritis Nodosa,
Microscopic Polyangiitis, and Churg-Strauss
Syndrome
Analysis of four prospective trials including 278
patients
Gayraud, Martine, Guillevin, Loic Arthritis
Rheumatism March 2001

38
Study Method

pts w PAN, MPA, CCS studied prospectively for
prognostic factors
most were randomized into 5 treatment protocols
age 15-75
clinical dx histologic evidence or
arteriographic evidence or fulfillment of ACR
criteria

39
Protocol 1 -PO cyclo

1980-1983
Prednisone/ PE vs. Prednisone/ PE oral cyclo
Pred 1mg/kg X 1mon, then tapered
PE 3X 1st wk, 2X 2nd wk, 1X per wk X 4, 1Xper
month X4
oral cyclo -2mg/kg /d X1yr
did not take into account HBV status
stopped in 1983, began protocols 2 and 5

40
Protocol 2 -PE? (1983-1988)

pts without HBV infection included
pred PE vs. pred alone
cyclo PO used if failure of assigned rx
PE 3X per wk for 2wks, 2X for 1wk, 1 session 10,
15, 21, 30d later

41
Protocol 3 ?PE in severe PAN (89-93)

(no HBV) at least one of
age gt50
GI tract involvement
cardiomyopathy
renal insufficiency Crgt 140 or GN
CNS involvement
WCB gt 12
Pred / IV cyclo / PE vs. Pred/ IV cyclo
IV cyclo 0.6mg/m2 monthly pulse

42
Protocol 4 PO vs IV cyclo

PAN (no HBV), no factors of poor prognosis
pred po cyclo vs pred IV cyclo

43
Protocol 5 Hep B -PAN

corticosteroids X 2wks
PE and vidarabine
interferon alpha 2b
more to follow

44
Results
45
Results - Univariate Analysis
46
Results -Multivariate Analysis
47
Results -5 yr Mortality
48
Limitations

heterogenous group with different diseases
in the past treated the same way
even HBV related PAN included
did not take into account differences in
treatment
different efficacy
different side effects
they later show prognosis quite similar for these
diseases

49
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50
Follow-up Report

278 pts
mean age at dx 53.8 /- 15yrs
54.3 M, 45.7 F
mean follow up 7yrs /- 52 months
CCS 64
MPA 58
PAN 93
HBV PAN 63

51
Survival - FFS
52
Survival - Type of Vasculitis
53
Relapses

20 experienced
not correlated w FFS or use of cytotoxic agents
(23 vs. 24)
type of vasculitis HBV - PAN (7.9), PAN
(19.4), CCS (20.3), MPA (34.5)
time to relapse similar for all types (24-37
months)

54
Deaths
55
Deaths

41 (of 85) pts died as consequence of vasculitis
or treatment
22 died uncontrolled vasculitis
11 died s/e sepsis
6 sudden death
2 sequelae of cardiomyopathy
18 of 22 pts who died of uncontrolled vasculitis
had poor prognostic factors

56
CS vs. CS Cyclo
57
FFSgt2 CS vs. CS Cyclo
P 0.044
58
Side Effects

93 of 278 (35)
85 had received Cyclo
infectious disease (31 of 37 had cyclo)
osteoporotic fractures 8.6 (14 of 24 had cyclo)
all 11 pts who died of sepsis had taken Cyclo
oral cyclo 59, IV cyclo 62 had s/e
none had major s/e in hepB PAN protocol

59
ConclusionsCS vs. CS Cyclo

no difference in survival overall
Cyclo prolonged survival in FFS scores gt2
(p0.044)
of 22 who died of uncontrolled vasculitis, 15
took CS alone
Cyclo did not prevent relapse
side effects were more frequent in cyclo group,
especially infectious complications
only one case of bladder ca attributed to cyclo

60
Conclusions oral vs. IV Cyclo

protocol 4, 25 patients, good prognosis (no FFS)
no significant difference
IV pulse cyclo increasingly used, small trials
less hemorrhagic cystitis, bladder hematologic
malignancies, lower cumulative dose
case reports of oral cyclo being effective after
IV pulse has failed to control activity

Gayraud M, Luillevin L et al. Treatment of
goo-prognosis polyarteritis nodosa and
Churg-Strauss syndomre comparison of steroids
and oral or pulse cyclophosphamide in 25
patients. Br J Rheumatol 1997 36
1290-7. Genereau T et al. Treatment of systemic
vasculitis with cyclophosphamide and steroids
daily oral low-dose cyclophosphamide
administration after failure of a pulse
intravenous high-dose regimen in four patients.
Br J Rheumatol 1994 33959-62. Adu D et al.
Controlled trial of pulse vs. continuous
prednisolone and cyclophosphamide in the
treatment of systemic vasculitis. QJM 1997 90
401-9.
61
Conclusions Plasma Exchanges (no Hep B)

62 pts with severe PAN (FFS) (protocol 3)
no difference in 5 yr survival (75 PE, 88
without)
78pts with non-selected PAN, only used cyclo for
failed initial rx
no difference 7 yr survival (83 PE, 79 without)
PE as 2nd line rx with PAN refractory to therapy

Guillevin L et al. Lack of superiority of
steroids puls plasma exchanges to steroids alone
int eh treatment of polyarteritis nodosa and
Churg-Strauss syndrome a prospective, randomized
trial in 78 patients. Arthritis Rheum 1992
35208-15. Guillevin L et al. Corticosteroids
plus pulse cyclophosphamide and plasma exchanges
vs. corticosteroids plus pulse cyclophosphamide
alone in the treatment of polyarteritis nodosa
and Chur-Strauss syndrome patients with factors
predicting poor prognosis a prospective,
randomized trial in sixty-two patients. Arthritis
Rheum 1995 38 1638-45.
62
Limitations

though studies prospective, randomized, very
small
not enough power to exclude differences
probably does not apply to MPA/ WG who have
necrotizing glomerulonephritis
cyclophosphamide still treatment of choice (MTX
also been used)

63
Treatment of hep B related PAN

corticosteroids and immunosuppressive agents
perpetuate chronic hepatitis B infection and
facilitate progression to cirrhosis
survival rates at one year significantly lower in
pts with HBs antigenemia than without (70 vs.
85)
heightened mortality related to GI complications,
including GI bleeding and perforations, more
frequently found in HBV associated polyarteritis

64
Protocol 5, HBV

study effectiveness of antiviral agents used in
association with short-term immunosuppression
included HBsAg and HBeAg , active replication
shown by HBV DNA
initial CS to control vasculitis activity, then
anti-viral agents to treat hepatitis B while
using PE to suppress disease activity without
immunosuppresion

65
Protocol 5, HBV

Pred 1mg/kg/d X1wk, tapered X1wk - stop
if clinical remission/ failure, continue pred
X1wk, then try to taper
Vidarabine X 3wks after stopping pred IV infusion
repeat if HBeAg did not seroconvert within 4mon
PE 3X/wk for 2wks, 4X during vidarabine wk1, 5X
during 2nd and 3rd
3X /wk for 3wks, 2X/wk for 2wks, then 1-2X/wk
then stopped depending on clinical

66
Protocol 5, HBV

1987 -interferon-alpha 2b used as second line
agent if failure of HBeAg seroconversion
early 1990s -interferon-alpha 2b used as first
line agent instead of vidarabine
3million units, 3X/wk for max of 1yr

67
Results

41 pts followed 35 vidarabine, 6 IFN alph2b
10 yr survival rate 83
HBeAg/ HBeAb servoconversion in 21 or 41
total viral clearance HBsAg/HBsAb seroconversion
in 10 (24)
vidarabine only used X3 wks because of
neurotoxicity

Guillevin L, Lhote F et al. Polyarteritis nodosa
related to hepatitis B virus a prospective study
with long-term observation of 41 patients.
Medicine (Baltimore) 1995 74238-53.
68
Interferon alpha 2b

more effective antiviral against Hep B
case reports of successful therapy for PAN
replaced vidarabine

Avsar E, et al. Successful treatment of
polyarteritis nodosa related to hepatitis B virus
with interferon alpha as first-line therapy. J
Hepatology 1998 28 525-526. Simsek H, et al.
Successful treatment of hepatitis B
virus-associated polyarteritis nodosa by
interferon alpha alone. J Clin Gastroenterol
1995 20 263-265.
69
Lamivudine

nucleoside analogue, selectively inhibits reverse
transcriptase
first discovered in HIV/ HBV pts
reduction of 3-4 log HBV DNA in 1st 3 mons
associated w HBeAg loss, improved AST/ALT
well tolerated, therefore replacing IFN alpha

Ganem D. Hepatitis B virus infection - Natural
history and clinical consequences. NEJM 2004
3501118
70
Lamivudine

elevated ALT pretreatment predicts good response
(adequate host immune response)
reduces viral load, allowing host immune system
to deal more effectively with remaining infected
hepatocytes
limitation drug resistance mediated by mutations
at catalytic center of viral RT
1 yr 15-20 resistance, 40 at 2yrs, 67 at 4
yrs

71
Lamivudine in HepB PAN

now being used as first line anti-viral agents
for hep B-PAN, along w steroids /- PE or
cyclophosphamide
several case reports published, including NEJM
CPC
some case reports used anti-viral agents alone
but severity of vasculitis usually mandates
treatment w steroids
lamivudine used 6-12mons until HBeAg conversion,
HBV DNA titres down, HBsAg conversion

Coblyn J, McCluskey RT. Case 3-2003 a
36-year-old man with renal failure, hypertension,
and neurologic abnormalities. NEJM 2003
348333 Maclachlan D, Battegay M. Successful
treatment of hepatitis B-associated polyarteritis
nodosa with a combination of lamivudine and
conventional immunosuppressive therapy a case
report. Rheumatology 2000 39106-8.
72
Conclusion

treatment of PAN
corticosteroids to control vasculitis activity
cyclophosphamide for serious organ involvement or
failure to control activity with steroids alone
no evidence to support plasmaphoresis
treatment of hep B- PAN
corticosteroids to control vasculitis activity
cyclophosphamide may also be needed if CS alone
fails
lamivudine /other anti hep B rx
role of PE?

73
Back to Case