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Plasma exchange in rheumatoid vasculitis
09553886/92 $5.00+0.00 Copyright @J 1992 Pergamon Press plc
Transfus. Sci. 1992; 13:119-123 Printed in Great Britain. All rights reserved
Plasma Exchange in Rheumatoid Vasculitis Rui Clemente Coelho Miguel Lea1 Galvgo
n Rheumatoid vasculitis (RV) is a rare but severe complication of rheumatoid arthritis, affecting skin, nerves and internal organs; it is usually treated with Plasma immunosuppressive drugs. exchange (PE) was combined with methylprednisolone and cyclophosphamide in 3 women with RV. Stabilization of peripheral necrotic lesions was accomplished in all patients and the one suffering from Mononeuritis Multiplex had a moderate improvement. We reviewed the literature on diagnosis and treatment of RV and found 30 patients reported as treated with PE alone or in combined therapy; according to classifiable data (28 cases), we concluded that PE is particularly suitable to patients unable to undergo immunosuppression or with life-threatening forms of RV. n
other selected conditions,’ patients may benefit from PE: these include rheumatoid vasculitis (RV), a severe complication of classical rheumatoid arthritis (RA),3, 4 which is usually associated with significant morbidity (cutaneous iecrosis5 and polyneuropathy6 and a high mortality rate (30%).‘, ’ The theoretical basis for PE treatment in autoimmune disorders is to remove immune complexes and inflammatory mediators from blood, with subsequent microcirculation and dessaturation of the clearance9 mononuclear-phagocytic system; lo,I’ PE must be combined with immunosuppressive therapy in order to downself-reacting regulate lymphocyte clones. This paper describes 3 patients with RV treated with PE plus methylprednisolone (MP) and cyclophosphamide (CPP) and reviews 25 of the 30 cases reported in the literature managed by pE
9, 12-19
INTRODUCTION MATERIALS AND METHODS
Plasma exchange (PE) has been accepted as a good treatment modality in well defined clinical situations: hyperviscosity syndrome, thrombotic thrombocytopenic purpura, myasthenia gravis, crescentic glomerulonephritis with renal insufficiency, Goodpasture’s syndrome, familial hypercholesterolemia, l and acute Guillain-Barre syndrome.2 In some
hmuno-Haemotherapy Department, Hospital Maria, Av. Prof. Egas Moniz, Lisbon, Portugal. Received 6/91; Accepted 8/91.
There are 30 RV patients reported in the literature, whose therapy included PE. We will analyze those cases with classifiable data (25) and our 3 patients, which we describe here: Case No. 1 A 65yr-old woman had nodular RA for 14 yr. In January 1983 she was admitted to hospital because she developed digital necrosis, purporic lesions on feet and
de Santa
119
120
Transfus. Sci.
Vol. 13. No. 1
mononeuritis multiplex (MM) on lower limbs. Daily immunosuppressive therapy ( 100 mg MP plus 50 mg CPP) was immediately started and after a week the patient was enrolled in a PE program: five sessions of I.3 plasma volume exchange were performed in 20 days, using fresh frozen plasma as replacing solution. A clear delimitation of necrotic areas and a neurologic improvement occurred in 3 weeks. Case No. 2 A 75 yr-old woman was diagnosed of RA in April 1986; since then the disease had been erosive, with strongly positive serology. In November 1986 ischaemic lesions appeared on hands and feet, and evolved quickly to distal necrosis on 8 fingers. She was given immunosuppressive therapy (100 mg MP plus 100 mg CPP) and submitted to seven sessions of 1.3 plasma volume exchange (4% albumin) in 17 days. The stabilization of the necrotic border and the remission of purpuric nodules, led to discontinuing of PE. Case No. 3 A 63 yr-old woman had had deforming and erosive RA for 13 yr, being poorly controlled with corticosteroids. In October 1987 she noticed mild signs of cutaneous vasculitis on her right foot, which progressed rapidly to necrosis of one finger. Combined therapy of PE and daily immunosuppressive drugs (60 mg MP plus 150 mg CPP) was instituted. The apheresis protocol was performed on 13 days: six sessions of 0.9 plasma volume exchange using 4% albumin as replacing solution. Ischaemic and trophic changes were controlled after 2 weeks treatment, avoiding amputation. subsequent Erythrocyte sedimentation rate, Creactive Protein and rheumatoid factor, all became normal. The method we used to evaluate literature reports was to review all patients with respect to the following
criteria: RA characterization, presentation of indications for PE, frequency and associated therapy, laboratory monitoring and clinical results.
RESULTS RA Characterization Classical RA manifestations in patients developing systemic vasculitis were present in most patients: long disease duration (17.5 yr), severe articular damage (69% ), occurrence of rheumatoid nodules (65%) and strongly positive serology (73%) (Table 1). Presentation
of RV
The most common clinical features observed were: gangrene extremity (64%), skin ulcers (57%)‘ polyneuropathy (50%) and purpuric nodules (3 1%) (Table 2). PE Indications 15 were treated with PE for intractable disease, 3 for corticosteroid resistance, 2 for cryoglobulinemia and one for marrow depression secondary to cyclophosphamide. PE Schedule Scott, Duquesnoy, Bjelle and Coelho followed a PE schedule consisting in a short-term intensive program followed by a maintenance protocol, only varying in the plasma volume exchanged. Roux and Goldman group varied PE method among patients, and some also received several treatments in the first week. Associated Therapy According to reported data, 15 patients were medicated with MP plus CPP, 5 with MP alone, 3 with CPP alone and 2 with azathioprine. Three groups describe 5 patients managed by PE without associated therapy.
121
PE in Rheumatoid Vasculitis
Table 1.
Rheumatoid
Arthritis:
9 Articular damage Rheumatoid nodules Strongly positive n/n = ND =
2/2 ND ND
ND 3/4 4/4
ND 819 ND
Forms of Presentation
Gangrene of extremities PolvneuroDathv Pu&oric ioduies Skin ulcers
15
16
*
Total
ND II2 212
II2 212 l/2
416 216 II2
213 l/3 l/3
9113 (69%) 17/26 (65%) 11/E (73%)
of Rheumatoid
Total
Vasculitis
9
12
13
14
15
16
l
II2 l/2 O/2 l/2
314 314 ND 214
619 619 ND 619
l/2 II2 o/2 212
212 o/2 l/2 l/2
316 216 216 l/6
213 l/3 II3 313
18128 14/28 4/13 16128
(64%) (SO%] (31%) (57%)
patients affected/patients reported per parameter. non determined.
Laboratory
arteries are major targets of inflammatory process; however venules and capillaries may also be involved in milder forms of disease.22 Schneider et ~1.~ divides RV in two subtypes: type I, which includes mononeuritis multiplex and gangrene and type II which includes all other manifestations of RV. Most authors describe it as a rare complication of long-lasting RA, 23,24affecting patients with rheumatoid nodules25 and strongly positive serology. 26 The underlying physiopathological mechanism consists in immune complex deposition in the microcirculation,27, 28 leading to activation of neutrophils,29 platelets,30 macrophages31 and T-lymphocytes.’ The final deleterious event in tissues is probably related to free oxygen radicals and tumor necrosis factor-a (TNF-a). The management of RV is controversia14, ’ as with many autoimmune disorders. Scott and Bacon32 treated 100 patients with intermittent boluses of MP plus CPP and concluded this drug regimen led to healing and lowered relapse
Monitoring
No special laboratory parameters were used to monitor respopnse to PE procedures: erythrocyte sedimentation rate was mentioned by 5 groups, rheumatoid factor by six, complement consumption by three and immune complexes by two. Clinical Response Most authors were not very explicit about clinical evaluation after the PE program was started, but an accurate evaluation of available data shows that 55% of patients improved, 36% achieved stabilization, 23% had no response and 14% died (Table 3). DISCUSSION Vasculitic syndromes have been difficult to classify,20, 21 both from a clinical and histological point of view. Bacon’ includes RV in systemic necrotizing arteritis, where medium-size and small Table 3.
Clinical Response 9
Improvement Stabilization Ab response Death n/n =
14
patients affected/patients reported per parameter. non determined.
Table 2.
n/n = ND =
Features 12 13
Clinical
patients evaluated/patients
12
212
13
14
15
16
212
l/2 l/2
l/6 316 l/6 II6
719 214 2l4
2l9
reported per group.
l
l/3 213
Total 12l22 8l22 5/22 3/22
(55%) (36%) (23%) (14%)
122
Transfus. Sci. Vol. 13, No. 1
and mortality rates (in agreement with former results by Fauci et ~1.~~and Abel et ~1.~~). Schneider et ~1.~ states that aggressive therapy should be reserved for life-threatening situations like gangrene, mononeuritis multiplex, renal failure and polyserositis. Milder RV forms can be treated more conservatively as they tend to respond well to conventional therapy.35 The group of Goldman12 was the first to introduce PE in the management of RV (1979); carried out an empirical basis on that occasion, its role is still not totally clarified. No randomized controlled study with PE alone has been reported, and only occasional cases have been reported. 9, 17,28,31 A total of 8 patients have been described and all except one improved or achieved clinical stabilization. Our patients, treated with combined therapy, obtained a relatively good outcome, confirming previous reports. This literature review does not permit any clear-cut conclusions as no standard procedures were followed by the various groups. Our personal view about RV is that PE should be reserved for patients who cannot undergo immunosuppressive therapy (namely corticosteroids), those affected by very severe conditions (gangrene and/or mononeuritis multiplex) and for cases complicated by cryoglobulinemia.
6.
7.
8.
9.
10.
11.
12.
13.
14.
15.
REFERENCES 16.
(Moore BP, 1. Standards in Haemapheresis ed). ISBT Guide, Paris, 1986, 13 pp. 2. The Guillain-Barre Syndrome Study Group. Plasmapheresis and acute Guillain-Barre Syndrome. NeUKOlOgy 1985; 35: 1096. 3. Schneider H, Yonker RA, Katz P, Panush RS: Rheumatoid vasculitis: experience with 13 patients and review of the literature. Semin Arthritis Rheum 1985; 14(4):280-286. 4. Scott DGI, Bacon PA, Tribe CR: Systemic rheumatoid vasculitis: a clinical and laboratorial study of 50 cases, Medicine 1981; 60:288-297. FR, Cooper NS, Ziff M, 5. Schmidt
17.
18.
McEwen C: Arteritis in rheumatoid arthritis. Am J Med 1961; 3056-59. Krause VT, Wagner A, Hantzsched H: Incidence of neuropathies in so-called RV. ZGesamte InnMed 1986; 41(6):170172. Bacon PA: Vasculitis-clinical aspects and therapy. Acta Med Stand 1986; 715(Suppl.):157-163. Wilkinson M, Torrance WN: Clinical background of rheumatic vascular disease. Ann Rheum Dis 1961; 26:475-478. Bjelle A, Cedergren B, Wahlby L: Plasma exchange in two patients with rheumatoid vasculitis. Stand 1 Rheum 1981; 11:58-62. Lockwood CM, Worlledge S, Nicholas A: Reversal of impaired splenic function in patients with nephritis or vasculitis (or bothj by plasma exchange. N Engl / Med 1979; 300:524-530. Walport MJ, Peters AM, Elkon KB, Persey CD, Lavender JP, Hughes GR: The splenit extraction ratio of antibody-coated erythrocytes and its response to plasma exchange and pulse methylprednisolone. C1in Exp Immunol 1985; 60(3):465+73. Goldman JA, Casey HL, Mcllwain H, Kirby J, Wilson CH Jr, Miller SB: Limited plasmapheresis in rheumatoid arthritis with vasculitis. Arthritis Rheum 1979; 10:11461159. Scott DGI, Bacon PA, Bothamley JE, Allen C, Elson CJ, Wallington TB: Plasma exchange in rheumatoid vasculitis. 1 Rheum 1981; 8(3):433439. Brubaker DB, Winrelstein A: Plasma exchange in rheumatoid vasculitis. VOX Sang 1981; 41:295301. Duquesnoy B, Dracon M, BonnefoyCudraz M, Gaborit P, Givaudan JP, Lelievre G: Polyarthrite rheumatoide et vascularite necrosante extensive. Rev Rheum 1982; 49(5):371-375. Roux H, Gaborit P, Bonnefoy-Cudraz M, Deslour-Paoli MP, Fouquet B, Nowakovitch G: Exchanges plasmatiques et polyarthrites rheumatoides avec vascularite. A propos de six observations. Rev Rheum 1983; 50(2):105-109. Sakamoto H, Takaoka T, Usami M, Emura M, Okabe K, Matsushita M, Smith JN, Malchesky PS, Nose Y: Apheresis: clinical response to patients unresponsive to conventional therapy. Trans Am Sot Artif Intern Organs 1985; 31:704710. Itoh M, Endo S, Fukuma N, Furrauchi M, Kisamori S, Hirooka Y, Nihei, N, Yamazaki N: Effective plasma exchange for a patient with malignant rheumatoid
PE in Rheumatoid Vasculitis
19.
20.
21.
22. 23.
24.
25.
26.
27.
arthritis complicated with polyneuritis: a case report Nippon Naika Gakkai Zasshi 1985; 74( 11):307-313. Nuver Zwart I-W, Boerbooms AM, de Witte TJ: Plasma exchange in a patient with severe rheumatoid arthritis complicated by mononeuritis multiplex and cutaneous ulcers. Neth I Med 1986; 29(3):79-83. Fauci AS, Haynes BF, Katz P: The spectrum of vasculitis. Ann Intern Med 1978; 84:660-676. Alarcon-Segovia D: Classification of the necrotizing vasculitis in man. Clin Rheum Dis 1980; 6:223-232. Scott DGI, Bacon PA: Rheumatoid vasculitis. Clin Rheum 1983; 2(4):312-314. Panush RS, Katz P, Longley S, Carter R, Love J, Stanley H: Rheumatoid vasculitis: diagnostic and therapeutical decisions. Clin Rheum 1983; 2(4):321-330. Vollestrem RS, Corm DL, Ballard DJ, Ilstrup DM, Kazmar RE, Silverfield JC: Rheumatoid vasculitis: survival and associated risk factors. Medicine 1986; 65(6):365-375. Sokoloff L, Bunim JJ: Vascular lesions in rheumatoid arthritis. I Chron Dis 1957; 5:668487. Epstein WV, Engleman EP: The relations of the rheumatoid factor content of the serum to clinical neurovascular manifestations of rheumatoid arthritis. Arthritis Rheum 19.59; 2:250-258. Starz TW, Medsger TA, Ersenbeir CH: Sural nerve biopsies in rheumatoid arthritis: light microscopic and immune-
28.
29.
30.
31.
32.
33.
34.
35.
123
fluorescence findings in 13 patients. Arthritis Rheum 1978; 21:823-824. Corm DL, McDuffie FC, Dick PJ: Immunopathological study of sural nerves in rheumatoid arthritis. Arthritis Rheum 1979; 15:135-143. Breedveld FC, Heurkens AH, Lafeber GJ, Van Hinsbergh VW, Cats A: Immune complexes in sera from patients with rheumatoid vasculitis induce polymorphonuclear cell-mediated injury to endothelial cells. Clin Immunol lmmunopathol 1988; 48(2):202-213. Cunningham TJ, Medcalf RL, Mathews JD, Muirden KD: Platelet releasing activity in sera of patients with rheumatoid vasculitis. Ann Rheum Dis 1986; 45(1):15-20. Cavender LE, Haskand DO, Joseph B, et al. : Interleukin 1 increases the binding of human B and T lymphocytes to endotheha1 cell monolayers. / Immunol 1986; 136:203-207. Scott DGI, Bacon PA: Intravenous cyclophosphamid plus methilprednisolone in treatment of systemic rheumatoid vasculitis. Am / Med 1984; 76:377-384. Fauci AS, Katz P, Haynes BF: Cyclophosphamid therapy of severe systemic necrotizing vasculitis. N Engl I Med 1979; 301(5):235-238. Abel T, Andrews BS, Cunningham PH, BruMer CM, Davies JS, Horwitz DA: Ann Intern Med 1980: 93:407-413. Jaffe IA: The treatment of RA and necrotizing vasculitis with penicillamine. Arthritis Rheum 1970; 13:436-443.
Transfus. Sci. 1992; 13:119-123 Printed in Great Britain. All rights reserved
Plasma Exchange in Rheumatoid Vasculitis Rui Clemente Coelho Miguel Lea1 Galvgo
n Rheumatoid vasculitis (RV) is a rare but severe complication of rheumatoid arthritis, affecting skin, nerves and internal organs; it is usually treated with Plasma immunosuppressive drugs. exchange (PE) was combined with methylprednisolone and cyclophosphamide in 3 women with RV. Stabilization of peripheral necrotic lesions was accomplished in all patients and the one suffering from Mononeuritis Multiplex had a moderate improvement. We reviewed the literature on diagnosis and treatment of RV and found 30 patients reported as treated with PE alone or in combined therapy; according to classifiable data (28 cases), we concluded that PE is particularly suitable to patients unable to undergo immunosuppression or with life-threatening forms of RV. n
other selected conditions,’ patients may benefit from PE: these include rheumatoid vasculitis (RV), a severe complication of classical rheumatoid arthritis (RA),3, 4 which is usually associated with significant morbidity (cutaneous iecrosis5 and polyneuropathy6 and a high mortality rate (30%).‘, ’ The theoretical basis for PE treatment in autoimmune disorders is to remove immune complexes and inflammatory mediators from blood, with subsequent microcirculation and dessaturation of the clearance9 mononuclear-phagocytic system; lo,I’ PE must be combined with immunosuppressive therapy in order to downself-reacting regulate lymphocyte clones. This paper describes 3 patients with RV treated with PE plus methylprednisolone (MP) and cyclophosphamide (CPP) and reviews 25 of the 30 cases reported in the literature managed by pE
9, 12-19
INTRODUCTION MATERIALS AND METHODS
Plasma exchange (PE) has been accepted as a good treatment modality in well defined clinical situations: hyperviscosity syndrome, thrombotic thrombocytopenic purpura, myasthenia gravis, crescentic glomerulonephritis with renal insufficiency, Goodpasture’s syndrome, familial hypercholesterolemia, l and acute Guillain-Barre syndrome.2 In some
hmuno-Haemotherapy Department, Hospital Maria, Av. Prof. Egas Moniz, Lisbon, Portugal. Received 6/91; Accepted 8/91.
There are 30 RV patients reported in the literature, whose therapy included PE. We will analyze those cases with classifiable data (25) and our 3 patients, which we describe here: Case No. 1 A 65yr-old woman had nodular RA for 14 yr. In January 1983 she was admitted to hospital because she developed digital necrosis, purporic lesions on feet and
de Santa
119
120
Transfus. Sci.
Vol. 13. No. 1
mononeuritis multiplex (MM) on lower limbs. Daily immunosuppressive therapy ( 100 mg MP plus 50 mg CPP) was immediately started and after a week the patient was enrolled in a PE program: five sessions of I.3 plasma volume exchange were performed in 20 days, using fresh frozen plasma as replacing solution. A clear delimitation of necrotic areas and a neurologic improvement occurred in 3 weeks. Case No. 2 A 75 yr-old woman was diagnosed of RA in April 1986; since then the disease had been erosive, with strongly positive serology. In November 1986 ischaemic lesions appeared on hands and feet, and evolved quickly to distal necrosis on 8 fingers. She was given immunosuppressive therapy (100 mg MP plus 100 mg CPP) and submitted to seven sessions of 1.3 plasma volume exchange (4% albumin) in 17 days. The stabilization of the necrotic border and the remission of purpuric nodules, led to discontinuing of PE. Case No. 3 A 63 yr-old woman had had deforming and erosive RA for 13 yr, being poorly controlled with corticosteroids. In October 1987 she noticed mild signs of cutaneous vasculitis on her right foot, which progressed rapidly to necrosis of one finger. Combined therapy of PE and daily immunosuppressive drugs (60 mg MP plus 150 mg CPP) was instituted. The apheresis protocol was performed on 13 days: six sessions of 0.9 plasma volume exchange using 4% albumin as replacing solution. Ischaemic and trophic changes were controlled after 2 weeks treatment, avoiding amputation. subsequent Erythrocyte sedimentation rate, Creactive Protein and rheumatoid factor, all became normal. The method we used to evaluate literature reports was to review all patients with respect to the following
criteria: RA characterization, presentation of indications for PE, frequency and associated therapy, laboratory monitoring and clinical results.
RESULTS RA Characterization Classical RA manifestations in patients developing systemic vasculitis were present in most patients: long disease duration (17.5 yr), severe articular damage (69% ), occurrence of rheumatoid nodules (65%) and strongly positive serology (73%) (Table 1). Presentation
of RV
The most common clinical features observed were: gangrene extremity (64%), skin ulcers (57%)‘ polyneuropathy (50%) and purpuric nodules (3 1%) (Table 2). PE Indications 15 were treated with PE for intractable disease, 3 for corticosteroid resistance, 2 for cryoglobulinemia and one for marrow depression secondary to cyclophosphamide. PE Schedule Scott, Duquesnoy, Bjelle and Coelho followed a PE schedule consisting in a short-term intensive program followed by a maintenance protocol, only varying in the plasma volume exchanged. Roux and Goldman group varied PE method among patients, and some also received several treatments in the first week. Associated Therapy According to reported data, 15 patients were medicated with MP plus CPP, 5 with MP alone, 3 with CPP alone and 2 with azathioprine. Three groups describe 5 patients managed by PE without associated therapy.
121
PE in Rheumatoid Vasculitis
Table 1.
Rheumatoid
Arthritis:
9 Articular damage Rheumatoid nodules Strongly positive n/n = ND =
2/2 ND ND
ND 3/4 4/4
ND 819 ND
Forms of Presentation
Gangrene of extremities PolvneuroDathv Pu&oric ioduies Skin ulcers
15
16
*
Total
ND II2 212
II2 212 l/2
416 216 II2
213 l/3 l/3
9113 (69%) 17/26 (65%) 11/E (73%)
of Rheumatoid
Total
Vasculitis
9
12
13
14
15
16
l
II2 l/2 O/2 l/2
314 314 ND 214
619 619 ND 619
l/2 II2 o/2 212
212 o/2 l/2 l/2
316 216 216 l/6
213 l/3 II3 313
18128 14/28 4/13 16128
(64%) (SO%] (31%) (57%)
patients affected/patients reported per parameter. non determined.
Laboratory
arteries are major targets of inflammatory process; however venules and capillaries may also be involved in milder forms of disease.22 Schneider et ~1.~ divides RV in two subtypes: type I, which includes mononeuritis multiplex and gangrene and type II which includes all other manifestations of RV. Most authors describe it as a rare complication of long-lasting RA, 23,24affecting patients with rheumatoid nodules25 and strongly positive serology. 26 The underlying physiopathological mechanism consists in immune complex deposition in the microcirculation,27, 28 leading to activation of neutrophils,29 platelets,30 macrophages31 and T-lymphocytes.’ The final deleterious event in tissues is probably related to free oxygen radicals and tumor necrosis factor-a (TNF-a). The management of RV is controversia14, ’ as with many autoimmune disorders. Scott and Bacon32 treated 100 patients with intermittent boluses of MP plus CPP and concluded this drug regimen led to healing and lowered relapse
Monitoring
No special laboratory parameters were used to monitor respopnse to PE procedures: erythrocyte sedimentation rate was mentioned by 5 groups, rheumatoid factor by six, complement consumption by three and immune complexes by two. Clinical Response Most authors were not very explicit about clinical evaluation after the PE program was started, but an accurate evaluation of available data shows that 55% of patients improved, 36% achieved stabilization, 23% had no response and 14% died (Table 3). DISCUSSION Vasculitic syndromes have been difficult to classify,20, 21 both from a clinical and histological point of view. Bacon’ includes RV in systemic necrotizing arteritis, where medium-size and small Table 3.
Clinical Response 9
Improvement Stabilization Ab response Death n/n =
14
patients affected/patients reported per parameter. non determined.
Table 2.
n/n = ND =
Features 12 13
Clinical
patients evaluated/patients
12
212
13
14
15
16
212
l/2 l/2
l/6 316 l/6 II6
719 214 2l4
2l9
reported per group.
l
l/3 213
Total 12l22 8l22 5/22 3/22
(55%) (36%) (23%) (14%)
122
Transfus. Sci. Vol. 13, No. 1
and mortality rates (in agreement with former results by Fauci et ~1.~~and Abel et ~1.~~). Schneider et ~1.~ states that aggressive therapy should be reserved for life-threatening situations like gangrene, mononeuritis multiplex, renal failure and polyserositis. Milder RV forms can be treated more conservatively as they tend to respond well to conventional therapy.35 The group of Goldman12 was the first to introduce PE in the management of RV (1979); carried out an empirical basis on that occasion, its role is still not totally clarified. No randomized controlled study with PE alone has been reported, and only occasional cases have been reported. 9, 17,28,31 A total of 8 patients have been described and all except one improved or achieved clinical stabilization. Our patients, treated with combined therapy, obtained a relatively good outcome, confirming previous reports. This literature review does not permit any clear-cut conclusions as no standard procedures were followed by the various groups. Our personal view about RV is that PE should be reserved for patients who cannot undergo immunosuppressive therapy (namely corticosteroids), those affected by very severe conditions (gangrene and/or mononeuritis multiplex) and for cases complicated by cryoglobulinemia.
6.
7.
8.
9.
10.
11.
12.
13.
14.
15.
REFERENCES 16.
(Moore BP, 1. Standards in Haemapheresis ed). ISBT Guide, Paris, 1986, 13 pp. 2. The Guillain-Barre Syndrome Study Group. Plasmapheresis and acute Guillain-Barre Syndrome. NeUKOlOgy 1985; 35: 1096. 3. Schneider H, Yonker RA, Katz P, Panush RS: Rheumatoid vasculitis: experience with 13 patients and review of the literature. Semin Arthritis Rheum 1985; 14(4):280-286. 4. Scott DGI, Bacon PA, Tribe CR: Systemic rheumatoid vasculitis: a clinical and laboratorial study of 50 cases, Medicine 1981; 60:288-297. FR, Cooper NS, Ziff M, 5. Schmidt
17.
18.
McEwen C: Arteritis in rheumatoid arthritis. Am J Med 1961; 3056-59. Krause VT, Wagner A, Hantzsched H: Incidence of neuropathies in so-called RV. ZGesamte InnMed 1986; 41(6):170172. Bacon PA: Vasculitis-clinical aspects and therapy. Acta Med Stand 1986; 715(Suppl.):157-163. Wilkinson M, Torrance WN: Clinical background of rheumatic vascular disease. Ann Rheum Dis 1961; 26:475-478. Bjelle A, Cedergren B, Wahlby L: Plasma exchange in two patients with rheumatoid vasculitis. Stand 1 Rheum 1981; 11:58-62. Lockwood CM, Worlledge S, Nicholas A: Reversal of impaired splenic function in patients with nephritis or vasculitis (or bothj by plasma exchange. N Engl / Med 1979; 300:524-530. Walport MJ, Peters AM, Elkon KB, Persey CD, Lavender JP, Hughes GR: The splenit extraction ratio of antibody-coated erythrocytes and its response to plasma exchange and pulse methylprednisolone. C1in Exp Immunol 1985; 60(3):465+73. Goldman JA, Casey HL, Mcllwain H, Kirby J, Wilson CH Jr, Miller SB: Limited plasmapheresis in rheumatoid arthritis with vasculitis. Arthritis Rheum 1979; 10:11461159. Scott DGI, Bacon PA, Bothamley JE, Allen C, Elson CJ, Wallington TB: Plasma exchange in rheumatoid vasculitis. 1 Rheum 1981; 8(3):433439. Brubaker DB, Winrelstein A: Plasma exchange in rheumatoid vasculitis. VOX Sang 1981; 41:295301. Duquesnoy B, Dracon M, BonnefoyCudraz M, Gaborit P, Givaudan JP, Lelievre G: Polyarthrite rheumatoide et vascularite necrosante extensive. Rev Rheum 1982; 49(5):371-375. Roux H, Gaborit P, Bonnefoy-Cudraz M, Deslour-Paoli MP, Fouquet B, Nowakovitch G: Exchanges plasmatiques et polyarthrites rheumatoides avec vascularite. A propos de six observations. Rev Rheum 1983; 50(2):105-109. Sakamoto H, Takaoka T, Usami M, Emura M, Okabe K, Matsushita M, Smith JN, Malchesky PS, Nose Y: Apheresis: clinical response to patients unresponsive to conventional therapy. Trans Am Sot Artif Intern Organs 1985; 31:704710. Itoh M, Endo S, Fukuma N, Furrauchi M, Kisamori S, Hirooka Y, Nihei, N, Yamazaki N: Effective plasma exchange for a patient with malignant rheumatoid
PE in Rheumatoid Vasculitis
19.
20.
21.
22. 23.
24.
25.
26.
27.
arthritis complicated with polyneuritis: a case report Nippon Naika Gakkai Zasshi 1985; 74( 11):307-313. Nuver Zwart I-W, Boerbooms AM, de Witte TJ: Plasma exchange in a patient with severe rheumatoid arthritis complicated by mononeuritis multiplex and cutaneous ulcers. Neth I Med 1986; 29(3):79-83. Fauci AS, Haynes BF, Katz P: The spectrum of vasculitis. Ann Intern Med 1978; 84:660-676. Alarcon-Segovia D: Classification of the necrotizing vasculitis in man. Clin Rheum Dis 1980; 6:223-232. Scott DGI, Bacon PA: Rheumatoid vasculitis. Clin Rheum 1983; 2(4):312-314. Panush RS, Katz P, Longley S, Carter R, Love J, Stanley H: Rheumatoid vasculitis: diagnostic and therapeutical decisions. Clin Rheum 1983; 2(4):321-330. Vollestrem RS, Corm DL, Ballard DJ, Ilstrup DM, Kazmar RE, Silverfield JC: Rheumatoid vasculitis: survival and associated risk factors. Medicine 1986; 65(6):365-375. Sokoloff L, Bunim JJ: Vascular lesions in rheumatoid arthritis. I Chron Dis 1957; 5:668487. Epstein WV, Engleman EP: The relations of the rheumatoid factor content of the serum to clinical neurovascular manifestations of rheumatoid arthritis. Arthritis Rheum 19.59; 2:250-258. Starz TW, Medsger TA, Ersenbeir CH: Sural nerve biopsies in rheumatoid arthritis: light microscopic and immune-
28.
29.
30.
31.
32.
33.
34.
35.
123
fluorescence findings in 13 patients. Arthritis Rheum 1978; 21:823-824. Corm DL, McDuffie FC, Dick PJ: Immunopathological study of sural nerves in rheumatoid arthritis. Arthritis Rheum 1979; 15:135-143. Breedveld FC, Heurkens AH, Lafeber GJ, Van Hinsbergh VW, Cats A: Immune complexes in sera from patients with rheumatoid vasculitis induce polymorphonuclear cell-mediated injury to endothelial cells. Clin Immunol lmmunopathol 1988; 48(2):202-213. Cunningham TJ, Medcalf RL, Mathews JD, Muirden KD: Platelet releasing activity in sera of patients with rheumatoid vasculitis. Ann Rheum Dis 1986; 45(1):15-20. Cavender LE, Haskand DO, Joseph B, et al. : Interleukin 1 increases the binding of human B and T lymphocytes to endotheha1 cell monolayers. / Immunol 1986; 136:203-207. Scott DGI, Bacon PA: Intravenous cyclophosphamid plus methilprednisolone in treatment of systemic rheumatoid vasculitis. Am / Med 1984; 76:377-384. Fauci AS, Katz P, Haynes BF: Cyclophosphamid therapy of severe systemic necrotizing vasculitis. N Engl I Med 1979; 301(5):235-238. Abel T, Andrews BS, Cunningham PH, BruMer CM, Davies JS, Horwitz DA: Ann Intern Med 1980: 93:407-413. Jaffe IA: The treatment of RA and necrotizing vasculitis with penicillamine. Arthritis Rheum 1970; 13:436-443.