Globotriaosylceramide accumulation in the fabry kidney is cleared from multiple cell types after enzyme replacement therapy

Beth L. Thurberg; Helmut Rennke; Robert B. Colvin; Steven Dikman; Ronald E. Gordon; A. Bernard Collins; Robert J. Desnick; Michael O'Callaghan

doi:10.1046/j.1523-1755.2002.00675.x

Globotriaosylceramide accumulation in the fabry kidney is cleared from multiple cell types after enzyme replacement therapy

Beth L. Thurberg, Helmut Rennke, Robert B. Colvin, Steven Dikman, Ronald E. Gordon, A. Bernard Collins, Robert J. Desnick, Michael O'Callaghan

Research output: Contribution to journal › Article › peer-review

325 Scopus citations

Abstract

Background. Fabry disease, a lysosomal storage disease caused by deficient lysosomal α-galactosidase A activity, is characterized by globotriaosylceramide (GL-3) accumulation in multiple cell types, particularly the vasculature, leading to end organ failure. Accumulation in the kidney is responsible for progressive decline in renal function in male patients with the classical phenotype, resulting in renal failure in their third to fifth decades of life. With the advent of recombinant protein synthesis technology, enzyme replacement therapy has become a viable alternative to dialysis or renal transplantation, previously the only available treatment options for end-stage renal disease. Methods. The pre- and post-treatment renal biopsies were analyzed from fifty-eight Fabry patients enrolled in a Phase 3 double-blind, randomized, placebo-controlled trial followed by a six-month open label extension study of the recombinant human enzyme, α-galactosidase A (r-hαGalA), administered IV at 1 mg/kg biweekly. The purpose of this investigation was to detail the pathologic changes in glycosphingolipid distribution and the pattern of post-treatment clearance in the kidney. Results. Baseline evaluations revealed GL-3 accumulations in nearly all renal cell types including vascular endothelial cells, vascular smooth muscle cells, mesangial cells and interstitial cells, with particularly dense accumulations in podocytes and distal tubular epithelial cells. After 11 months of r-hαGalA treatment there was complete clearance of glycolipid from the endothelium of all vasculature as well as from the mesangial cells of the glomerulus and interstitial cells of the cortex. Moderate clearance was noted from the smooth muscle cells of arterioles and small arteries. Podocytes and distal tubular epithelium also demonstrated evidence for decreased GL-3, although this clearance was more limited than that observed in other cell types. No evidence of immune complex disease was found by immuno-fluorescence despite circulating anti-r-hαGalA IgG antibodies. Conclusions. These findings indicate a striking reversal of renal glycosphingolipid accumulation in the vasculature and in other renal cell types, and suggest that long-term treatment with r-hαGalA may halt the progression of pathology and prevent renal failure in patients with Fabry disease.

Original language	English
Pages (from-to)	1933-1946
Number of pages	14
Journal	Kidney International
Volume	62
Issue number	6
DOIs	https://doi.org/10.1046/j.1523-1755.2002.00675.x
State	Published - 2002

Keywords

End-stage renal disease
Fabry disease
Phase 3 trial
Renal disease
Renoprotection
X-linked recessive disorder, neutral glycosphingolipids

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10.1046/j.1523-1755.2002.00675.x

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@article{5986b934c33040d682c381cae778a4af,

title = "Globotriaosylceramide accumulation in the fabry kidney is cleared from multiple cell types after enzyme replacement therapy",

abstract = "Background. Fabry disease, a lysosomal storage disease caused by deficient lysosomal α-galactosidase A activity, is characterized by globotriaosylceramide (GL-3) accumulation in multiple cell types, particularly the vasculature, leading to end organ failure. Accumulation in the kidney is responsible for progressive decline in renal function in male patients with the classical phenotype, resulting in renal failure in their third to fifth decades of life. With the advent of recombinant protein synthesis technology, enzyme replacement therapy has become a viable alternative to dialysis or renal transplantation, previously the only available treatment options for end-stage renal disease. Methods. The pre- and post-treatment renal biopsies were analyzed from fifty-eight Fabry patients enrolled in a Phase 3 double-blind, randomized, placebo-controlled trial followed by a six-month open label extension study of the recombinant human enzyme, α-galactosidase A (r-hαGalA), administered IV at 1 mg/kg biweekly. The purpose of this investigation was to detail the pathologic changes in glycosphingolipid distribution and the pattern of post-treatment clearance in the kidney. Results. Baseline evaluations revealed GL-3 accumulations in nearly all renal cell types including vascular endothelial cells, vascular smooth muscle cells, mesangial cells and interstitial cells, with particularly dense accumulations in podocytes and distal tubular epithelial cells. After 11 months of r-hαGalA treatment there was complete clearance of glycolipid from the endothelium of all vasculature as well as from the mesangial cells of the glomerulus and interstitial cells of the cortex. Moderate clearance was noted from the smooth muscle cells of arterioles and small arteries. Podocytes and distal tubular epithelium also demonstrated evidence for decreased GL-3, although this clearance was more limited than that observed in other cell types. No evidence of immune complex disease was found by immuno-fluorescence despite circulating anti-r-hαGalA IgG antibodies. Conclusions. These findings indicate a striking reversal of renal glycosphingolipid accumulation in the vasculature and in other renal cell types, and suggest that long-term treatment with r-hαGalA may halt the progression of pathology and prevent renal failure in patients with Fabry disease.",

keywords = "End-stage renal disease, Fabry disease, Phase 3 trial, Renal disease, Renoprotection, X-linked recessive disorder, neutral glycosphingolipids",

author = "Thurberg, {Beth L.} and Helmut Rennke and Colvin, {Robert B.} and Steven Dikman and Gordon, {Ronald E.} and Collins, {A. Bernard} and Desnick, {Robert J.} and Michael O'Callaghan",

note = "Funding Information: This work was supported in part by grants from the National Institutes of Health including a research grant (R29 DK 34045 Merit Award), a grant (5 MO1 RR00071) for the Mount Sinai General Clinical Research Center Program from the National Center of Research Resources, a grant (5 P30 HD28822) for the Mount Sinai Child Health Research Center, and a research grant from the Genzyme Corporation. Many thanks to the Genzyme Pathology Department staff for their help in developing a histologic grading system, to the Medical Information Department for their help with extensive literature searches on Fabry Disease, and to Biometrics for statistical data analysis. We also thank the clinical investigators and their patients at the multiple sites who participated in this trial: C.M. Eng, M. Banikazemi, J. Ibraham, and A.P. Cheng ( New York, NY, USA ); W.R. Wilcox and L.J. Raffel ( Los Angeles, CA, USA ); N. Guffon and P. Cochat ( Lyon, France ); D.P. Germain, M. Azizi, and X. Jeunemaitre ( Paris, France ); P. Lee and A. Vellodi ( London, UK ); S. Waldek and J.E. Wraith ( Manchester, UK ); L. Caplan, C.J. Chaves, K.B. Kanis, I. Linfante, and R. Llinas ( Boston, MA, USA ); and C.E.M. Hollak, G.E. Linthorst, D.K. Bosman, H.S.A. Heymans, and F.A. Wijburg ( Amsterdam, The Netherlands ).",

year = "2002",

doi = "10.1046/j.1523-1755.2002.00675.x",

language = "English",

volume = "62",

pages = "1933--1946",

journal = "Kidney International",

issn = "0085-2538",

publisher = "Elsevier B.V.",

number = "6",

}

TY - JOUR

T1 - Globotriaosylceramide accumulation in the fabry kidney is cleared from multiple cell types after enzyme replacement therapy

AU - Thurberg, Beth L.

AU - Rennke, Helmut

AU - Colvin, Robert B.

AU - Dikman, Steven

AU - Gordon, Ronald E.

AU - Collins, A. Bernard

AU - Desnick, Robert J.

AU - O'Callaghan, Michael

N1 - Funding Information: This work was supported in part by grants from the National Institutes of Health including a research grant (R29 DK 34045 Merit Award), a grant (5 MO1 RR00071) for the Mount Sinai General Clinical Research Center Program from the National Center of Research Resources, a grant (5 P30 HD28822) for the Mount Sinai Child Health Research Center, and a research grant from the Genzyme Corporation. Many thanks to the Genzyme Pathology Department staff for their help in developing a histologic grading system, to the Medical Information Department for their help with extensive literature searches on Fabry Disease, and to Biometrics for statistical data analysis. We also thank the clinical investigators and their patients at the multiple sites who participated in this trial: C.M. Eng, M. Banikazemi, J. Ibraham, and A.P. Cheng ( New York, NY, USA ); W.R. Wilcox and L.J. Raffel ( Los Angeles, CA, USA ); N. Guffon and P. Cochat ( Lyon, France ); D.P. Germain, M. Azizi, and X. Jeunemaitre ( Paris, France ); P. Lee and A. Vellodi ( London, UK ); S. Waldek and J.E. Wraith ( Manchester, UK ); L. Caplan, C.J. Chaves, K.B. Kanis, I. Linfante, and R. Llinas ( Boston, MA, USA ); and C.E.M. Hollak, G.E. Linthorst, D.K. Bosman, H.S.A. Heymans, and F.A. Wijburg ( Amsterdam, The Netherlands ).

PY - 2002

Y1 - 2002

N2 - Background. Fabry disease, a lysosomal storage disease caused by deficient lysosomal α-galactosidase A activity, is characterized by globotriaosylceramide (GL-3) accumulation in multiple cell types, particularly the vasculature, leading to end organ failure. Accumulation in the kidney is responsible for progressive decline in renal function in male patients with the classical phenotype, resulting in renal failure in their third to fifth decades of life. With the advent of recombinant protein synthesis technology, enzyme replacement therapy has become a viable alternative to dialysis or renal transplantation, previously the only available treatment options for end-stage renal disease. Methods. The pre- and post-treatment renal biopsies were analyzed from fifty-eight Fabry patients enrolled in a Phase 3 double-blind, randomized, placebo-controlled trial followed by a six-month open label extension study of the recombinant human enzyme, α-galactosidase A (r-hαGalA), administered IV at 1 mg/kg biweekly. The purpose of this investigation was to detail the pathologic changes in glycosphingolipid distribution and the pattern of post-treatment clearance in the kidney. Results. Baseline evaluations revealed GL-3 accumulations in nearly all renal cell types including vascular endothelial cells, vascular smooth muscle cells, mesangial cells and interstitial cells, with particularly dense accumulations in podocytes and distal tubular epithelial cells. After 11 months of r-hαGalA treatment there was complete clearance of glycolipid from the endothelium of all vasculature as well as from the mesangial cells of the glomerulus and interstitial cells of the cortex. Moderate clearance was noted from the smooth muscle cells of arterioles and small arteries. Podocytes and distal tubular epithelium also demonstrated evidence for decreased GL-3, although this clearance was more limited than that observed in other cell types. No evidence of immune complex disease was found by immuno-fluorescence despite circulating anti-r-hαGalA IgG antibodies. Conclusions. These findings indicate a striking reversal of renal glycosphingolipid accumulation in the vasculature and in other renal cell types, and suggest that long-term treatment with r-hαGalA may halt the progression of pathology and prevent renal failure in patients with Fabry disease.

AB - Background. Fabry disease, a lysosomal storage disease caused by deficient lysosomal α-galactosidase A activity, is characterized by globotriaosylceramide (GL-3) accumulation in multiple cell types, particularly the vasculature, leading to end organ failure. Accumulation in the kidney is responsible for progressive decline in renal function in male patients with the classical phenotype, resulting in renal failure in their third to fifth decades of life. With the advent of recombinant protein synthesis technology, enzyme replacement therapy has become a viable alternative to dialysis or renal transplantation, previously the only available treatment options for end-stage renal disease. Methods. The pre- and post-treatment renal biopsies were analyzed from fifty-eight Fabry patients enrolled in a Phase 3 double-blind, randomized, placebo-controlled trial followed by a six-month open label extension study of the recombinant human enzyme, α-galactosidase A (r-hαGalA), administered IV at 1 mg/kg biweekly. The purpose of this investigation was to detail the pathologic changes in glycosphingolipid distribution and the pattern of post-treatment clearance in the kidney. Results. Baseline evaluations revealed GL-3 accumulations in nearly all renal cell types including vascular endothelial cells, vascular smooth muscle cells, mesangial cells and interstitial cells, with particularly dense accumulations in podocytes and distal tubular epithelial cells. After 11 months of r-hαGalA treatment there was complete clearance of glycolipid from the endothelium of all vasculature as well as from the mesangial cells of the glomerulus and interstitial cells of the cortex. Moderate clearance was noted from the smooth muscle cells of arterioles and small arteries. Podocytes and distal tubular epithelium also demonstrated evidence for decreased GL-3, although this clearance was more limited than that observed in other cell types. No evidence of immune complex disease was found by immuno-fluorescence despite circulating anti-r-hαGalA IgG antibodies. Conclusions. These findings indicate a striking reversal of renal glycosphingolipid accumulation in the vasculature and in other renal cell types, and suggest that long-term treatment with r-hαGalA may halt the progression of pathology and prevent renal failure in patients with Fabry disease.

KW - End-stage renal disease

KW - Fabry disease

KW - Phase 3 trial

KW - Renal disease

KW - Renoprotection

KW - X-linked recessive disorder, neutral glycosphingolipids

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U2 - 10.1046/j.1523-1755.2002.00675.x

DO - 10.1046/j.1523-1755.2002.00675.x

M3 - Article

C2 - 12427118

AN - SCOPUS:0036436320

SN - 0085-2538

VL - 62

SP - 1933

EP - 1946

JO - Kidney International

JF - Kidney International

IS - 6

ER -

Globotriaosylceramide accumulation in the fabry kidney is cleared from multiple cell types after enzyme replacement therapy

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Keywords

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