The management of pulmonary small vessel vasculitides

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The management of pulmonary small vessel vasculitides

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Title: The management of pulmonary small vessel vasculitides

1
The management of pulmonary small vessel
vasculitides

Dr. Aditya Jindal
www.jindalchest.com

55 years female
Cough with hemoptysis x 1month
Sputum AFB ve

EBB/TBLB/BAL-granulomatuous inflammtion with
neutrophilic infiltration
cANCA ve

59 y female
Hoarseness of voice x 1m
Fever x 1 m
Weight loss/ cough
Sputum AFB ve
TBLB/ BAL non specific inflammation
cANCA strongly ve

First patient
Given Cyclophosphamide steroid pulse
Initial recovery
Developed relapse after 4 months and died
Second patient
Given steroid pulse with methotrexate
Doing well with almost complete resolution of
lesions

The vasculitides are a set of related disorders
characterized by blood vessel inflammation
leading to tissue or end-organ injury
Differentiated from other vascular disorders by
the presence of inflammation of the vessel wall
as compared to bland vasculopathy

7
Frankel SK, Jayne D. The Pulmonary Vasculitides.
Clin Chest Med 31 (2010) 519536
8
(No Transcript)
9
Frankel SK, Jayne D. The Pulmonary Vasculitides.
Clin Chest Med 31 (2010) 519536
10
Clinical criteria for GPA, E-GPA, and MPA
Arman et al. Int J Nephrol Renovasc Dis. 2018
11
Management
12

Not much difference between different types of
vasculitis
Most trials of GPA, treatment extrapolated to
other types
Divided into remission-induction and maintenance
phases
Treatment stratified according to severity

13
Mukhtyar C etal. EULAR recommendations for the
management of primary small and medium vessel
vasculitis. Ann Rheum Dis 200968310317.
14

Remission induction

15
Frankel SK, Jayne D. The Pulmonary Vasculitides.
Clin Chest Med 31 (2010) 519536
16

A. Localised disease
Refers to isolated upper or lower airway disease
and a complete absence of other end organ
involvement or constitutional symptoms
Managed with topical therapy, corticosteroids,
and/or a single moderate potency cytotoxic agent
such as methotrexate or azathioprine

B. Early generalized disease
Presence of constitutional symptoms and active
vasculitis but without any specific threat to
organ function
Standard therapy ? Azathiprine/ Methotrexate/
Cylophosphamide steroids
C. Generalized active disease
Presence of constitutional symptoms and
threatened organ function caused by vasculitic
activity
Standard therapy ? Cylophosphamide steroids

D. Severe disease
Presence or threat of immediate organ failure
and/or death
Rapidly progressive glomerulonephritis and renal
failure (creatinine gt5.7 mg/dL)
Alveolar hemorrhage associated with respiratory
failure
Cardiomyopathy with heart failure
Life-threatening arrhythmias
Central nervous system disease
Gastrointestinal disease with bowel schemia or
life-threatening hemorrhage
Standard treatment ? Plasma exchange i/v
cyclophophamide steroids

19
Induction Trials in AAV
Lee et al. Pediatric Rheumatology. 2019
20

Oral cyclophosphamide plus steroids ? standard
therapy since the 1970s
CYCLOPS (Daily Oral Versus Pulse Cyclophosphamide
for Renal Vasculitis) trial
149 patients with newly diagnosed generalized
active AAV (GPA or MPA) were randomized to pulse
intravenous cyclophosphamide (15 mg/kg every 2
weeks x first 3 doses, then every 3 weeks for
next 3 -6 doses) or daily oral cyclophosphamide
(2 mg/kg/d) plus prednisolone

No difference in time to remission or proportion
of patients who achieved remission (88.1 vs
87.7 at 9 months) or survival or renal function
Pulse group had a lower rate of leukopenia and
received a lower total cumulative dose of
cyclophosphamide
de Groot K, Harper L, Jayne DR, et al. Pulse
versus daily oral cyclophosphamide for induction
of remission in antineutrophil cytoplasmic
antibody-associated vasculitis a randomized
trial. Ann Intern Med 2009150670

NORAM (Non-Renal Alternative with Methotrexate)
trial
Compared methotrexate with cyclophosphamide for
the induction of remission in early disease
95 patients (89 with GPA and 6 with MPA)
MTx dose ? 15 mg /week escalating to 20 25
mg/week
Time to remission (5 m vs 3 m)
Relapse rate (74 vs 42) favored
cyclophosphamide
Methotrexate was better tolerated and had less
side affects
de Groot K, Rasmussen N, Bacon PA, et al.
Randomized trial of cyclophosphamide versus
methotrexate for induction of remission in early
systemic antineutrophil cytoplasmic
antibody-associated vasculitis. Arthritis Rheum
2005522461

Mycophenolate mofetil (MMF)
3 RCTS
First compared MMF 2g/day to ivCYC
35 participants (34 GPA, 1 MPA)
Exclusions
severe renal failure
life-threatening organ manifestations (lung
haemorrhage, central nervous system involvement)
14 of 18 patients (77.8) treated with MMF and 8
of 17 patients (47.1) receiving CYC had complete
remission
Second MMF 1- 1.5 g/d vs CYC monthly pulses
41 patients (all MPA)
Complete remission achieved in 63.6 of the CVYC
group and 78.9 of the MMF group

Third - MYCYC (MMF versus CYC for remission
induction of AAV)
MMF (2-3 g/d) vs iv CYC
Complete remission in 67 in MMF group vs 61 in
CYC group
relapses occurred significantly more frequently
with MMF (33) compared to ivCYC (19)
Hu W, Liu C, Xie H, Chen H, Liu Z, Li L.
Mycophenolate mofetil versus cyclophosphamide for
inducing remission of ANCA vasculitis with
moderate renal involvement. Nephrology, dialysis,
transplantation official publication of the
European Dialysis and Transplant Association -
European Renal Association. 2008 Apr
23(4)1307-1312.
Han F, Liu G, Zhang X, Li X, He Q, He X, et al.
Effects of mycophenolate mofetil combined with
corticosteroids for induction therapy of
microscopic polyangiitis. American journal of
nephrology. 2011 33(2)185-192.
Jones RB, Hiemstra TF, Ballarin J, Blockmans DE,
Brogan P, Bruchfeld A, et al. Mycophenolate
mofetil versus cyclophosphamide for remission
induction in ANCA-associated vasculitis a
randomised, non-inferiority trial. Ann Rheum Dis.
201978(3)399405

Methotrexate / MMF (indications)
in the absence of renal involvement
Nasal and paranasal disease without bony
involvement (erosion) or cartilage collapse or
olfactory dysfunction or deafness
Skin involvement without ulceration
Myositis (skeletal muscle only)
Non-cavitating pulmonary nodules/infiltrate
without haemoptysis
When cyclophosphamide or rituximab are not
available or contraindicated or patient choice

Methotrexate / MMF contraindications
Meningeal involvement
Retro-orbital disease
Cardiac involvement
Mesenteric involvement
Acute-onset mononeuritis multiplex
Pulmonary haemorrhage of any severity

MEPEX (Plasma Exchange or High-Dosage
Methylprednisolone as Adjunctive Therapy for
Severe Renal Vasculitis)
EUVAS sponsored randomised controlled trial
137 patients with a new diagnosis of AAV and a
serum creatinine level greater than 500 mmol/L
(5.7 mg/dL) were included
All patients received standard therapy with oral
cyclophosphamide and oral prednisolone and were
then randomized to either 7 plasma exchanges or
3000 mg of intravenous methylprednisolone
Primary end point ? ESRD or death at 3 m

At 3m ? 69 of patients treated with plasma
exchange were alive and independent of dialysis
compared with only 49 in the methylprednisolone
group
No significant benefit on long term follow up
(composite end point of ESRD and death)
Jayne DRW, Gaskin G, Rasmussen N, et al.
Randomised trial of plasma exchange or high dose
methyl prednisolone as adjunctive therapy for
severe renal vasculitis. J Am Soc Nephrol 2007
182180
Walsh M, Casian A, Flossmann O, Westman K,
Hoglund P, Pusey C, et al. Long-term follow-up of
patients with severe ANCA-associated vasculitis
comparing plasma exchange to intravenous
methylprednisolone treatment is unclear. Kidney
international. 2013 Aug 84(2)397-402
A 20 patient case series showed the efficacy of
this treatment strategy in alveolar hemorrhage
also
Klemmer PJ, Chalermskulrat W, Reif MS, et al.
Plasmapheresis therapy for diffuse alveolar
hemorrhage in patients with small vessel
vasculitis. Am J Kidney Dis 2003421149

PEXIVAS (Plasma exchange and glucocorticoid
dosing in the treatment of ANCA-associated
vasculitis)
704 patients with 7 year follow up
Compared Plasma exchange with no plasma exchange
Also standard dose with reduced dose steroids
(lt60)
Composite end point of ESRD and death
289 (41) PR3-ANCA, 209 (59) MPO-ANCA
691 (98) with renal involvement 191 (27) with
alveolar hemorrhage
109 (15) patients received rituximab and 595
(85) received cyclophosphamide

Primary outcome 31 in no plasma exchange group
and 28 in plasma exchange group
Primary outcome in 28 in reduced steroid group
and 26 in standard dose group
Less infections in reduced steroid group
www.pexivas.bham.ac.uk, http//clinicaltrials.gov/
ct2/show/NCT00987389
Walsh M, Merkel PA, Jayne D. The Effects of
Plasma Exchange and Reduced-Dose Glucocorticoids
during Remission-Induction for Treatment of
Severe ANCA-Associated Vasculitis
abstract. Arthritis Rheumatol. 2018 70 (suppl
10).

Rituximab
Targets the CD20 antigen on the surface of B
cells and clears circulating B cells from the
circulation
RAVE (Rituximab in ANCA-Associated Vasculitis)
trial
Multicenter, randomized, double-blind,
double-dummy, noninferiority trial, 197 patients
Compared rituximab with po CYC followed by AZA
for the induction of complete remission by 6
months in patients with severe ANCA-associated
vasculitis
64 of the patients achieved complete remission
compared to 53 in the cyclophosphamide control
arm

More efficacious than the cyclophosphamide-based
regimen for inducing remission of relapsing
disease 34 of 51 patients in the rituximab group
(67) as compared with 21 of 50 patients in the
control group (42) (P 0.01)
As effective as cyclophosphamide in the treatment
of patients with major renal disease or alveolar
hemorrhage
No significant differences between the treatment
groups with respect to rates of adverse events
Remission rates lower than other trials (earlier
discontinuation of steroids)
Long term follow up In severe AAV without organ
failure RTX better at maintaining remission
after 18 m
Stone JH, Merkel PA, Spiera R et al. Rituximab
versus cyclophosphamide for ANCA-associated
vasculitis. N Engl J Med 2010 36322132

RITUXVAS (rituximab versus cyclophosphamide in
ANCA associated vasculitis) trial
44 patients with newly diagnosed ANCA-associated
vasculitis and renal involvement were randomly
assigned, in a 31 ratio, to a standard
glucocorticoid regimen plus
either rituximab at a dose of 375 mg/sqm/week for
4 weeks, with two intravenous cyclophosphamide
pulses (33 patients, the rituximab group)
or intravenous cyclophosphamide for 3 to 6 months
followed by azathioprine (11 patients, the
control group)
More severe disease than RAVE trial
76 patients in the rituximab group and 82
patients in the control group had a sustained
remission (P 0.68)

Severe adverse events occurred in 14 patients in
the rituximab group (42) and 4 patients in the
control group (36) (P 0.77)
Rituximab-based regimen was not superior to
standard intravenous cyclophosphamide for severe
ANCA-associated vasculitis
Sustained-remission rates were high in both
groups
Rituximab-based regimen was not associated with
reductions in early severe adverse events
Jones RB, Tervaert JW,Hauser T et al. Rituximab
versus cyclophosphamide in ANCA-associated renal
vasculitis. N Engl J Med 2010 36321120

E. Refractory disease
Disease that does not respond to conventional
accepted therapy
Investigational or unproven therapies are used
Infliximab - chimeric IgGk monoclonal antibody
against soluble and membrane-bound TNF
Has given positive benefit in small trials

b. Anti thymocyte globulin
Studied in the EUVAS sponsored SOLUTION trial
15 patients received ATG for refractory
vasculitis
Partial disease remission was induced in 9/15 and
complete disease remission in 4/15
2 patients died after drug administration
1 of pulmonary hemorrhage
1 of infection
Serum sickness and nonfatal infections were among
the notable complications
Schmitt WH etal. Treatment of refractory
Wegener's granulomatosis with antithymocyte
globulin (ATG) an open study in 15 patients.
Kidney Int. 2004 Apr65(4)1440-8

Intravenous immunoglobulin (IVIg)
Studied in small clinical trials
Effect is generally short-lived
Most appropriate in acute situations where
conventional therapy is contraindicated
especially if severe infection is present
WEGENT (Wegeners Granulomatosis-Entretien) trial
32 induction-refractory (24 WG and 8 MPA)
patients were treated with oral CYC in 20
patients, combined with infliximab in 1
15 (75) achieved remission or low disease
activity state, 3 subsequently died of
uncontrolled disease and 2 entered remission
using several other agents including biological
agents
Seror R, Pagnoux C, Ruivard M, et al. Treatment
strategies and outcome of induction-refractory
Wegeners granulomatosis or microscopic
polyangiitis analysis of 32 patients with
first-line induction-refractory disease in the
WEGENT trial. Ann Rheum Dis 20106921252130
Alemtuzumab
Deoxyspergualin

Remission maintenance

39
Maintenance Trials in AAV
40
Lee et al. Pediatric Rheumatology. 2019
41

CYCAZAREM (Cyclophosphamide versus Azathioprine
for Remission in Generalized Vasculitis) trial
EUVAS sponsored randomised controlled trial
Patients were initially treated with oral
cyclophosphamide and oral prednisolone for
induction
They were then randomised to
Either oral cylophosphamide for 12 m followed by
azathioprine
Or directly to azathioprine
No difference in relapse rates (15.5 in the AZA
group and 13.7 in the CYC group) P 0.65 95
confidence interval (CI) -9.9 to13.0 up to the
end of the study at 18 months after treatment
outset
Jayne D, Rasmussen N, Andrassy K, et al. A
randomized trial of maintenance therapy for
vasculitis associated with antineutrophil
cytoplasmic autoantibodies. N Engl J Med 2003
34936.

IMPROVE (International Mycophenolate Mofetil to
Reduce Outbreaks of Vasculitides) trial
EUVAS sponsored Open-label randomized controlled
trial
Directly compared mycophenolate mofetil with
azathioprine for the maintenance of remission in
renal vasculitis
156 patients were assigned to azathioprine (n80)
or mycophenolate mofetil (n76) and followed up
for a median of 39 months

Relapses were more common in the mycophenolate
mofetil group (42/76 patients) compared with the
azathioprine group (30/80 patients), with an
unadjusted hazard ratio (HR) for mycophenolate
mofetil of 1.69 (95 confidence interval CI,
1.06-2.70 P.03)
Severe adverse events did not differ
significantly between groups
Hiemstra TF, Walsh M, Mahr A, et al European
Vasculitis Study Group (EUVAS). Mycophenolate
mofetil vs azathioprine for remission maintenance
in antineutrophil cytoplasmic antibody-associated
vasculitis a randomized controlled trial. JAMA
2010304(21)23812388

WEGENT trial
MTX vs AZA
126 participants with AAV (GPA 96 and MPA 30)
Patients randomised to either MTX or AZA after
pulse CYC (6 doses)
Given for 2 years and withdrawn
24 months after randomisation, relapse-free
survival rates were 71.8 in the AZA group and
74.5 in the MTX group
The hazard ratio for the risk of relapse among
MTX vs AZA was 0.92 (95 CI, 0.52 to 1.65 P
0.78)
Pagnoux C, Mahr A, Hamidou MA, Boffa JJ, Ruivard
M, Ducroix JP, et al. Azathioprine or
methotrexate maintenance for ANCA-associated
vasculitis. N Engl J Med. 2008

MAINRITSAN trial
115 participants with AAV (87 GPA, 23 MPA and
five with renal limited vasculitis)
Compared RTX to AZA
RTX given as 500 mg infusion at 0 and 2 weeks
followed by 6, 12 and 18 m
fewer major relapses at 28 months in the RTX
group compared with the AZA group (5 versus 29)
Long term follow up of 60 m showed superiority of
RTX with greater rates of relapse-free and
overall survival
Guillevin L, Pagnoux C, Karras A, Khouatra C,
Aumaitre O, Cohen P, et al. Rituximab versus
azathioprine for maintenance in ANCA-associated
vasculitis. N Engl J Med. 2014371

MAINRITSAN 2 trial
Compared an individually tailored RTX regimen
with fixed-schedule regimen
Tailored-infusion arm received RTX at
randomization and received repeat infusions based
on lymphocyte counts and ANCA titers until 18 m
Fix-scheduled arm received the same regimen from
the original MAINRITSAN trial
No significant difference between the number of
relapses but the tailored infusion arm received
fewer number of infusions
Charles P, Terrier B, Perrodeau E, Cohen P,
Faguer S, Huart A, et al. Comparison of
individually tailored versus fixed-schedule
rituximab regimen to maintain ANCA-associated
vasculitis remission results of a multicentre,
randomised controlled, phase III trial
(MAINRITSAN2). Ann Rheum Dis. 2018

47
(No Transcript)
48
Yates M, Watts RA, Bajema IM, et al. Ann Rheum
Dis 2016
49

Additional points
Dosage and schedule of cyclophosphamide
15 mg/kg (maximum 1.2 g) iv infusion every 2
weeks for first three doses f/b every 3 weeks for
next 3 6 doses
Dose adjustment can be made based on creatinine
levels
Oral prednisolone or prednisone at 1 mg/kg/day is
started alongside and maintained for 1 month, and
should not be reduced to less than 15 mg/day for
the first 3 months ?then tapered to a maintenance
dose of 10 mg/day or less during remission
When a rapid effect is needed, intravenous pulsed
methylprednisolone may be used in addition to the
oral prednisolone as part of remission induction
therapy

50
Protocol target prednisolone dosages
Yates M, Watts RA, Bajema IM, et al. Ann Rheum
Dis 2016
51

The addition of trimethoprim/sulphamethoxazole
(800/160 mg twice daily) to standard remission
maintenance can reduce the risk of relapse in WG
Prophylaxis against Pneumocystis jiroveci in all
patients being treated with cyclophosphamide
with trimethoprim/sulphamethoxazole (800/160 mg
on alternate days or 400/80 mg daily) is
recommended

Thromboembolic disease in the setting of AAV
The Wegeners Clinical Occurrence of Thrombosis
(WeCLOT) study identified that the incidence of
thromboembolic disease in patients with WG was
7.0 per 100 person-years, which is the same rate
of venous thromboembolic (VTE) disease as for
patients with a known prior history of VTE
Clinicians should consider patients with AAV to
be at higher risk for VTE
Merkel PA, Lo GH, Holbrook JT, et al. Brief
communication high incidence of venous
thrombotic events among patients with Wegener
granulomatosis the Wegeners Clinical Occurrence
of Thrombosis (WeCLOT) Study. Ann Intern Med
2005 142620

53
Yates M, Watts RA, Bajema IM, et al. Ann Rheum
Dis 2016
54

Alveolar hemorrhage(AH)
Defined as bilateral alveolar infiltrates on
radiological imaging without an alternative
explanation plus at least one of the following
Hemoptysis
Increased carbon monoxide diffusing capacity
Bronchoscopic evidence of hemorrhage
Unexplained drop in hemoglobin
Casian A, Jayne D. Management of Alveolar
Hemorrhage in Lung Vasculitides. Semin Respir
Crit Care Med 201132335345
Vasculitis was the third most common cause of AH
requiring intensive care support (19 of
patients), after thrombocytopenia (27) and
sepsis (22)
Rabe C, Appenrodt B, Hoff C, et al. Severe
respiratory failure due to diffuse alveolar
hemorrhage clinical characteristics and outcome
of intensive care. J Crit Care 201025(2) 230235

The majority (80) of these vasculitis cases with
AH are due to ANCA associated vasculitis (AAV)

Papiris SA, Manali ED, Kalomenidis I, Kapotsis
GE, Karakatsani A, Roussos C. Bench-to-bedside
review pulmonary-renal syndromesan update for
the intensivist.. Crit Care 200711(3)213
56

AH is the most common respiratory manifestation
of AAV, occurring in 24
Casian A, Jayne D. Management of Alveolar
Hemorrhage in Lung Vasculitides. Semin Respir
Crit Care Med 201132335345
AH appears similar in the PR3-ANCA and MPO ANCA
groups with regard to clinical features and
severity of respiratory failure
Mild AH is more common (in 24 to 28 of AAV)
28 of patients may retrospectively report
previous symptoms suggestive of AH for gt12 months
before diagnosis

Cyclophosphamide/rituximab glucocorticoids /-
Plasma exchange
Recombinant, activated factor VII ? useful in
case reports in life threatening, uncontrollable
AH
Henke D, Falk RJ, Gabriel DA. Successful
treatment of diffuse alveolar hemorrhage with
activated factor VII. Ann Intern Med
2004140(6)493494
Heslet L, Nielsen JD, Levi M, Sengeløv H,
Johansson PI. Successful pulmonary administration
of activated recombinant factor VII in diffuse
alveolar hemorrhage. Crit Care 200610(6)R177
Extracorporeal membrane oxygenation (ECMO)

Diagnosis -investigations -severity
Localised
Early systemic
Generalised
Severe
Refractory
Induction
Standard Steroids CYC
Ritux Steroids rituximab
59
Remission achieved
Maintenance
Standard Steroids AZA/ MTX
Rituximab Steroids RTX
Tailored
Scheduled
60
At the end

The prognosis of the pulmonary small vessel
vasculitides has improved markedly in the last
few years provided timely diagnosis is made and
adequate treatment instituted
Important to follow a structured clinical
assessment and treatment protocol
Long term follow up is required
Lots of new developments in the field