Interleukin-6 receptor inhibition with tocilizumab in various renal involvements associated with multicentric Castleman's disease: a report of three cases

doi:10.1093/ndtplus/sfn157

NDT Plus Advance Access originally published online on October 8, 2008
NDT Plus 2008 1(6):423-426; doi:10.1093/ndtplus/sfn157

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Interleukin-6 receptor inhibition with tocilizumab in various renal involvements associated with multicentric Castleman's disease: a report of three cases

Hirotaka Komaba¹, Takashi Nakazawa², Yutaka Yamaguchi³, Shunichi Kumagai² and Masafumi Fukagawa¹

¹ Division of Nephrology and Kidney Center
² Department of Clinical Pathology and Immunology, Kobe University School of Medicine, Kobe
³ Department of Pathology, Kashiwa Hospital, The Jikei University School of Medicine, Chiba, Japan

Correspondence: Correspondence and offprint requests to: Masafumi Fukagawa, Division of Nephrology and Kidney Center, Kobe University School of Medicine, 7-5-2 Kusunoki-cho, Chuo-ku, Kobe 650-0017, Japan. Tel: +81-78-382-6500; Fax: +81-78-382-6509; E-mail: fukagawa{at}med.kobe-u.ac.jp

Abstract

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Abstract
Introduction
Case reports
Discussion
References

Multicentric Castleman's disease (MCD) is an inflammatory lymphoproliferativedisorder characterized by polyclonal hypergammopathy and dysregulatedoverproduction of interleukin-6 (IL-6). A variety of renal involvementsinfrequently arise in patients with MCD. However, there is noestablished treatment for MCD and its associated renal involvements.We present the effects of an anti-IL-6 receptor monoclonal antibody,tocilizumab, on three patients with MCD associated with variousrenal manifestations. In all three patients, tocilizumab treatmentwas very effective in reducing proteinuria and stabilizing renalfunction, as well as improving other clinical symptoms. Thesefindings indicate the pathological significance of IL-6 in renalinvolvements associated with MCD, and the potential use of tocilizumabin its treatment.

Key Words: anti-interleukin-6 receptor antibody • interleukin-6 • multicentric Castleman's disease • tocilizumab

Received for publication September 13, 2008. Accepted for publication September 16, 2008.

Introduction

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Abstract
Introduction
Case reports
Discussion
References

Castleman's disease (CD), also known as angiofollicular lymphnode hyperplasia, is an uncommon lymphoproliferative disordercharacterized by benign lymphadenopathy and polyclonal hypergammopathy[1]. A multicentric form of CD (MCD) manifests systemicallyas fever, weight loss, anaemia, hypergammaglobulinaemia andhypoalbuminaemia. In addition, a variety of renal involvementsinfrequently arise in patients with MCD. However, there is noestablished treatment for MCD and its associated renal involvements.

Although the precise mechanism of MCD remains unknown, recentbasic and clinical studies have brought considerable advancesin our understanding of MCD, especially with regard to the roleof interleukin-6 (IL-6) and its receptor (IL-6R) [2]. Recently,a humanized anti-IL-6R monoclonal antibody, tocilizumab, hasbeen proved to be therapeutically effective for MCD [3]. Herewe present the effects of tocilizumab treatment in three patientswith MCD associated with various renal manifestations.

Case reports

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Abstract
Introduction
Case reports
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Patient 1
A 46-year-old man was admitted to our hospital because of generalfatigue, and generalized lymphadenopathy. Seven years beforeadmission, he had visited a local hospital because of tender,enlarged lymph nodes in the right inguinal region, for whichsurgical resection was performed. However, there was no improvementof the symptoms, and he was referred to our hospital for furtherinvestigation. On admission, the serum creatinine level was0.65 mg/dL, blood urea nitrogen was 10 mg/dL, haemoglobin was10.8 g/dL, total serum protein was 11.0 g/dL, serum albuminwas 2.0 g/ dL, and C-reactive protein (CRP) was 8.8 mg/dL. Urineanalysis showed microhaematuria and proteinuria of 1.0 g/ 24h. Serum protein electrophoresis results showed a polyclonalgammopathy with an increased level of IgG of 6070 mg/dL (IgG1,62%; IgG2, 23%; IgG3, 4% and IgG4, 11%). Serum IL-6 was markedlyelevated to 23.8 pg/mL. Collagen vascular disease workup wasnegative. We re-examined the specimens of the lymph nodes sentfrom the local hospital, which was compatible with the mixedtype of CD.

The renal biopsy showed a slightly thickened glomerular basementmembrane with a bubbly appearance, as observed by periodic acid–Schiff–methenaminesilver staining (Figure 1A). There was also a mild increasein mesangial matrix and cellularity. There was focal interstitialnephritis with infiltration of plasma cells and lymphocytes.Of note, the perirenal adipose capsule was dominated by massiveinfiltration of plasma cells and lymphocytes, showing follicle-likelymphoid strictures with interfollicular neovascularization(Figure 1B). An immunofluorescence study showed IgG2 depositsalong the capillary wall (Figure 1C). Electron microscopy showednumerous scattered subepithelial and intramembranous deposits(Figure 1D). These findings were consistent with membranousnephropathy (MN) associated with renal and perirenal plasmacell infiltration.

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Fig. 1 (A) The glomerular basement membrane is slightly thickened, with a bubbly appearance (periodic acid–Schiff–methenamine silver stain, original magnification x400). (B) Perirenal fat is dominated by massive infiltration of plasma cells and lymphocytes, showing follicle-like lymphoid strictures with interfollicular neovascularization (periodic acid–Schiff stain, original magnification x40). (C) Only IgG2 is positive; all other IgG subclasses are negative. (D) Numerous scattered subepithelial and intramembranous deposits are found. (E) Patchy infiltration of plasma cells and lymphocytes is observed in the interstitium (periodic acid–Schiff, original magnification x200). (F) Marked amyloid deposits are seen in the glomeruli and vascular walls (periodic acid–Schiff, original magnification x100).

He was treated with prednisolone 30 mg/day, but his symptomsand biochemical abnormalities were not improved. We, therefore,started intravenous tocilizumab 8 mg/kg every 2 weeks. After2 months of treatment, anaemia, hypoalbuminaemia, elevationof CRP and polyclonal gammopathy were all improved. Furthermore,his urine protein level decreased to <0.5 g/24 h (Figure2). Prednisolone therapy could be discontinued without exacerbation.He has been doing well with slight proteinuria and stable renalfunction.

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Fig. 2 Clinical response patterns in three patients treated with tocilizumab for up to 6 months.

Patient 2
A 53-year-old man was admitted to our hospital for evaluationof anaemia and generalized lymphadenopathy. He had been diagnosedwith diabetes mellitus 5 years ago, which was well managed withglibenclamide. On admission, the serum creatinine level was1.47 mg/dL, blood urea nitrogen was 19 mg/dL, haemoglobin was9.5 g/dL, total serum protein was 12.9 g/dL, serum albumin was1.7 g/dL and CRP was 13.7 mg/dL. Urine analysis showed microhaematuriaand proteinuria of 2.6 g/24 h. Serum protein electrophoresisresults showed a polyclonal gammopathy with an increased levelof IgG of 8680 mg/dL. Serum IL-6 was markedly elevated to 62.2pg/mL. Collagen vascular disease workup was negative. Therewas no evidence of diabetic retinopathy or neuropathy. Histologicalfindings of the right inguinal enlarged lymph nodes were compatiblewith the plasma cell type of CD.

The renal biopsy showed 10 glomeruli, 3 of which exhibited globalsclerosis. The remaining glomeruli showed diffuse mesangialstalk thickening and hyalinosis of both afferent and efferentarterioles. There was patchy infiltration of plasma cells andlymphocytes in the interstitium (Figure 1E). The immunofluorescencestudy showed no significant staining of glomeruli. Electron-densedeposits were absent. The biopsy findings were compatible withinterstitial nephritis associated with plasma cell infiltration,superimposed on pre-existing early diabetic glomerulosclerosis.

He was treated with 8 mg/kg tocilizumab intravenously every2 weeks without concomitant immunosuppression. Within 3 monthsof treatment, his anaemia, hypoalbuminaemia, inflammation andpolyclonal gammopathy were all improved. Furthermore, serumcreatinine and proteinuria decreased to 1.12 mg/dL and 0.4 g/24h, respectively (Figure 2). He has been free of symptoms withstabilized renal function for 1 year while maintained on tocilizumabtreatment.

Patient 3
A 54-year-old woman was admitted to our hospital because ofgeneral fatigue, chronic inflammation and generalized lymphadenopathyover 10 years. On admission, the serum creatinine level was1.00 mg/dL, blood urea nitrogen was 16 mg/dL, haemoglobin was10.0 g/dL, total serum protein was 10.1 g/dL, serum albuminwas 3.0 g/dL and CRP was 5.9 mg/dL. Urine analysis showed microhaematuriaand proteinuria of 1.7 g/24 h. Serum protein electrophoresisresults showed a polyclonal gammopathy with an increased levelof IgG of 4800 mg/dL. The antinuclear antibody was positiveat 1/80. Serum IL-6 was elevated to 20.4 pg/mL. Histologicalfindings of the left inguinal lymph nodes were compatible withthe plasma cell type of CD. The renal biopsy showed marked amyloiddeposits in the glomeruli and vascular walls (Figure 1F). Theimmunofluorescence study showed no significant staining of glomeruli.

She was treated with prednisolone 15–20 mg/day as an outpatient,but biochemical abnormalities, including proteinuria, were notimproved. She was then treated with 8 mg/kg tocilizumab intravenouslyevery 2 weeks. Surprisingly, she achieved complete remissiononly after 1 month of tocilizumab treatment. Within 3 monthsof treatment, her anaemia, hypoalbuminaemia, inflammation andpolyclonal gammopathy were improved. Renal function remainedstable (Figure 2). Prednisolone therapy was discontinued withoutexacerbation. She has been free of symptoms, with stabilizedrenal function.

Discussion

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Abstract
Introduction
Case reports
Discussion
References

Renal histopathological lesions associated with CD are veryheterogeneous, including mesangial proliferative glomerulonephritis[4], membranoproliferative glomerulonephritis (MPGN) [5], interstitialnephritis [6] and amyloidosis [7]. Here, we report three patientswith various MCD-related renal diseases, i.e., MN, interstitialnephritis with plasma cell infiltration and renal amyloidosis.Our experience with tocilizumab treatment and recent insightinto the pathological roles of IL-6 led to the hypothesis thatthis cytokine also contributes, either directly or indirectly,to the development of various renal involvements.

The direct action of IL-6 on renal involvements has been suggestedin experimental studies. IL-6 regulates mesangial cell growthin an autocrine manner [8], and IL-6 transgenic mice developmesangial proliferative glomerulonephritis and plasma cell infiltration[9]. These findings suggest that IL-6 plays a central role inthese types of nephritis. In addition, overproduction of IL-6may also induce plasma cells to infiltrate the kidneys, therebyleading to interstitial nephritis. A longstanding overproductionof the serum amyloid A protein induced by IL-6 may result inrenal amyloidosis. Furthermore, excessive expression of IL-6also causes the production of vascular endothelial growth factor(VEGF). The pathogenic role of VEGF in renal involvements remainsunknown [5]; however, given that tight regulation of VEGF signallingis critical for maintenance of the glomerular filtration barrier,local or systemic VEGF overproduction seems causative ratherthan protective.

Other pathogenic factors associated with IL-6 overproduction,such as polyclonal hypergammopathy and a variety of autoantibodies,may also be involved in the pathogenesis of CD-related renaldiseases. In this regard, the distribution pattern of IgG subclassesin MN is interesting; it has been shown to be biased towardsIgG4 in idiopathic MN and IgG3 in lupus-related MN [10]. Inour case of MN associated with MCD (Patient 1), IgG2 was theonly positive subclass in the glomeruli, despite its low circulatinglevel. Although the pathogenic role of IgG2 is unknown, thisfinding may suggest that our case of MN is a manifestation secondaryto MCD, rather than a coincidental occurrence of idiopathicMN.

The present case studies showed that blockade of IL-6 by tocilizumabwas therapeutically effective for various renal involvementsassociated with MCD, as well as improving other clinical symptomsrelated to MCD. These findings support the notion that IL-6plays, either directly or indirectly, a central role in thepathogenesis of various MCD-related renal diseases. Of note,Patient 3, who had severe renal amyloidosis, achieved completeremission of proteinuria only after 1 month of treatment. Becauseinsoluble amyloid depositions were unlikely to be cleared insuch a short time, we surmise that IL-6R inhibition may havedirectly restored glomerular capillary permeability, resultingin remission of proteinuria. Indeed, complete remission of nephroticsyndrome can be achieved after the removal of localized CD butwithout histological regression in renal amyloidosis [7].

In conclusion, tocilizumab is a very promising treatment forvarious renal involvements associated with MCD. This study alsoindicated the pathological significance of IL-6 in various renalinvolvements in CD. The response to tocilizumab for other renaldiseases is also of interest. Further clinical studies are neededto better evaluate the role of tocilizumab in the treatmentof renal diseases associated with IL-6 overproduction.

Acknowledgements

The authors thank Dr G. Tsuji, Dr H. Hayashi, Dr A. Abe andDr N. Yamanaka for thoughtful discussions, and all colleagueswho recorded medical information and performed renal biopsies.

Conflict of interest statement. None declared.

References

Top
Abstract
Introduction
Case reports
Discussion
References

Castleman B, Iverson L, Menendez VP. Localized mediastinal lymph node hyperplasia resembling thymoma. Cancer (1956) 9:822–830.[CrossRef][Web of Science][Medline]
Nishimoto N, Kishimoto T. Interleukin 6: from bench to bedside. Nat Clin Pract Rheumatol (2006) 2:619–626.[CrossRef][Web of Science][Medline]
Nishimoto N, Kanakura Y, Aozasa K, et al. Humanised anti-interleukin-6 receptor antibody treatment of multicentric Castlemans disease. Blood (2005) 106:2627–2632.[Abstract/Free Full Text]
Lui SL, Chan KW, Li FK, et al. Castleman's disease and mesangial proliferative glomerulonephritis: the role of interleukin-6. Nephron (1998) 78:323–327.[CrossRef][Web of Science][Medline]
Seida A, Wada J, Morita Y, et al. Multicentric Castleman's disease associated with glomerular microangiopathy and MPGN-like lesion: does vascular endothelial cell-derived growth factor play causative or protective roles in renal injury? Am J Kidney Dis (2004) 43:E3–E9.[Medline]
Frokjaer Thomsen O, Ladefoged J. Castleman's disease with renal infiltration by polyclonal plasma cells. Clin Nephrol (1998) 49:328–330.[Web of Science][Medline]
Keven K, Nergizoglu G, Ates K. Remission of nephrotic syndrome after removal of localized Castelman's disease. Am J Kidney Dis (2000) 35:1207–1211.[CrossRef][Web of Science][Medline]
Ruef C, Budde K, Lacy J, et al. Interleukin 6 is an autocrine growth factor for mesangial cells. Kidney Int (1990) 38:249–257.[Web of Science][Medline]
Brandt SJ, Bodine DM, Dunbar CE, et al. Dysregulated interleukin 6 expression produces a syndrome resembling Castleman's disease in mice. J Clin Invest (1990) 86:592–599.[Web of Science][Medline]
Haas M. IgG subclass deposits in glomeruli of lupus and nonlupus membranous nephropathies. Am J Kidney Dis (1994) 23:358–364.[Web of Science][Medline]

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