Immunologic, clinical, and radiologic status 14 months after cessation of natalizumab therapy

Olaf Stuve; P. D. Cravens; Elliot Frohman; J. T. Phillips; G. M. Remington; G. Von Geldern; S. Cepok; M. P. Singh; J. W. Cohen Tervaert; M. De Baets; D. MacManus; D. H. Miller; E. W. Radü; E. M. Cameron; Nancy L Monson; Song Zhang; R. Kim; B. Hemmer; M. K. Racke

doi:10.1212/01.wnl.0000327341.89587.76

Immunologic, clinical, and radiologic status 14 months after cessation of natalizumab therapy

Olaf Stuve, P. D. Cravens, Elliot Frohman, J. T. Phillips, G. M. Remington, G. Von Geldern, S. Cepok, M. P. Singh, J. W. Cohen Tervaert, M. De Baets, D. MacManus, D. H. Miller, E. W. Radü, E. M. Cameron, Nancy L Monson, Song Zhang, R. Kim, B. Hemmer, M. K. Racke

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Abstract

OBJECTIVE: Natalizumab is a humanized recombinant monoclonal antibody against very late activation antigen-4 approved for the treatment of patients with multiple sclerosis (MS). A phase II study failed to demonstrate a difference between natalizumab treatment groups and the placebo group with regard to gadolinium enhancing lesions on MRI 3 months after discontinuation of therapy. The objective of this study was to assess clinical MS disease activity, surrogate disease markers on MRI, immunologic parameters in peripheral blood and CSF, as well as safety in patients with MS after discontinuation of natalizumab therapy. METHODS: This study is a longitudinal and serial cross-sectional assessment, in which 23 patients who were treated with natalizumab in the context of two phase III clinical trials were originally enrolled. A subgroup of patients was followed over 14 months. The annual relapse rate, neurologic disease progression assessed by the Expanded Disability Status Scale, disease surrogate markers on MRI, cellular and humoral immune markers in peripheral blood and CSF, and adverse events of the drug were monitored. RESULTS: With regard to clinical disease activity, neuroimaging, and immune responses, the majority of patients in our cohort were stable. Decreased lymphocyte cell numbers and altered cell ratios returned to normal 14 months after cessation of natalizumab. No infectious complications were observed. CONCLUSION: This is the first long-term follow-up of patients who discontinued natalizumab. We did not observe a clinical, radiographic, or immunologic rebound phenomenon after discontinuation of natalizumab therapy.

Original language	English (US)
Pages (from-to)	396-401
Number of pages	6
Journal	Neurology
Volume	72
Issue number	5
DOIs	https://doi.org/10.1212/01.wnl.0000327341.89587.76
State	Published - Feb 3 2009

ASJC Scopus subject areas

Clinical Neurology

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Stuve, O., Cravens, P. D., Frohman, E., Phillips, J. T., Remington, G. M., Von Geldern, G., Cepok, S., Singh, M. P., Cohen Tervaert, J. W., De Baets, M., MacManus, D., Miller, D. H., Radü, E. W., Cameron, E. M., Monson, N. L., Zhang, S., Kim, R., Hemmer, B., & Racke, M. K. (2009). Immunologic, clinical, and radiologic status 14 months after cessation of natalizumab therapy. Neurology, 72(5), 396-401. https://doi.org/10.1212/01.wnl.0000327341.89587.76

Stuve, O, Cravens, PD, Frohman, E, Phillips, JT, Remington, GM, Von Geldern, G, Cepok, S, Singh, MP, Cohen Tervaert, JW, De Baets, M, MacManus, D, Miller, DH, Radü, EW, Cameron, EM, Monson, NL , Zhang, S, Kim, R, Hemmer, B & Racke, MK 2009, 'Immunologic, clinical, and radiologic status 14 months after cessation of natalizumab therapy', Neurology, vol. 72, no. 5, pp. 396-401. https://doi.org/10.1212/01.wnl.0000327341.89587.76

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title = "Immunologic, clinical, and radiologic status 14 months after cessation of natalizumab therapy",

abstract = "OBJECTIVE: Natalizumab is a humanized recombinant monoclonal antibody against very late activation antigen-4 approved for the treatment of patients with multiple sclerosis (MS). A phase II study failed to demonstrate a difference between natalizumab treatment groups and the placebo group with regard to gadolinium enhancing lesions on MRI 3 months after discontinuation of therapy. The objective of this study was to assess clinical MS disease activity, surrogate disease markers on MRI, immunologic parameters in peripheral blood and CSF, as well as safety in patients with MS after discontinuation of natalizumab therapy. METHODS: This study is a longitudinal and serial cross-sectional assessment, in which 23 patients who were treated with natalizumab in the context of two phase III clinical trials were originally enrolled. A subgroup of patients was followed over 14 months. The annual relapse rate, neurologic disease progression assessed by the Expanded Disability Status Scale, disease surrogate markers on MRI, cellular and humoral immune markers in peripheral blood and CSF, and adverse events of the drug were monitored. RESULTS: With regard to clinical disease activity, neuroimaging, and immune responses, the majority of patients in our cohort were stable. Decreased lymphocyte cell numbers and altered cell ratios returned to normal 14 months after cessation of natalizumab. No infectious complications were observed. CONCLUSION: This is the first long-term follow-up of patients who discontinued natalizumab. We did not observe a clinical, radiographic, or immunologic rebound phenomenon after discontinuation of natalizumab therapy.",

author = "Olaf Stuve and Cravens, {P. D.} and Elliot Frohman and Phillips, {J. T.} and Remington, {G. M.} and {Von Geldern}, G. and S. Cepok and Singh, {M. P.} and {Cohen Tervaert}, {J. W.} and {De Baets}, M. and D. MacManus and Miller, {D. H.} and Rad{\"u}, {E. W.} and Cameron, {E. M.} and Monson, {Nancy L} and Song Zhang and R. Kim and B. Hemmer and Racke, {M. K.}",

note = "Funding Information: Dr. St{\"u}ve was supported by a start-up grant from the Dallas VA Research Corporation, a New Investigator Award grant from VISN 17, Department of Veterans Affairs, a merit award from the Department of Veterans Affairs, research grants from National Multiple Sclerosis Society (NMSS; RG3427A8/T and RG2969B7/T), and a grant from the Viragh Foundation. Supported by grants (NS 37513 and NS 44250) from the NIH and NMSS grant RG 2969-B-7 to Dr. Racke. Drs. Hemmer and Cepok were supported by grants from the Deutsche Forschungsgemeinschaft (He 2386/4-2). Supported in part by the Adult AIDS Clinical Trials Group funded by the National Institute of Allergy and Infectious Diseases (AI 38858 and AI 27664). Dr. Monson was supported by a grant from the NIH (NS 40993). ",

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doi = "10.1212/01.wnl.0000327341.89587.76",

language = "English (US)",

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TY - JOUR

T1 - Immunologic, clinical, and radiologic status 14 months after cessation of natalizumab therapy

AU - Stuve, Olaf

AU - Cravens, P. D.

AU - Frohman, Elliot

AU - Phillips, J. T.

AU - Remington, G. M.

AU - Von Geldern, G.

AU - Cepok, S.

AU - Singh, M. P.

AU - Cohen Tervaert, J. W.

AU - De Baets, M.

AU - MacManus, D.

AU - Miller, D. H.

AU - Radü, E. W.

AU - Cameron, E. M.

AU - Monson, Nancy L

AU - Zhang, Song

AU - Kim, R.

AU - Hemmer, B.

AU - Racke, M. K.

N1 - Funding Information: Dr. Stüve was supported by a start-up grant from the Dallas VA Research Corporation, a New Investigator Award grant from VISN 17, Department of Veterans Affairs, a merit award from the Department of Veterans Affairs, research grants from National Multiple Sclerosis Society (NMSS; RG3427A8/T and RG2969B7/T), and a grant from the Viragh Foundation. Supported by grants (NS 37513 and NS 44250) from the NIH and NMSS grant RG 2969-B-7 to Dr. Racke. Drs. Hemmer and Cepok were supported by grants from the Deutsche Forschungsgemeinschaft (He 2386/4-2). Supported in part by the Adult AIDS Clinical Trials Group funded by the National Institute of Allergy and Infectious Diseases (AI 38858 and AI 27664). Dr. Monson was supported by a grant from the NIH (NS 40993).

PY - 2009/2/3

Y1 - 2009/2/3

N2 - OBJECTIVE: Natalizumab is a humanized recombinant monoclonal antibody against very late activation antigen-4 approved for the treatment of patients with multiple sclerosis (MS). A phase II study failed to demonstrate a difference between natalizumab treatment groups and the placebo group with regard to gadolinium enhancing lesions on MRI 3 months after discontinuation of therapy. The objective of this study was to assess clinical MS disease activity, surrogate disease markers on MRI, immunologic parameters in peripheral blood and CSF, as well as safety in patients with MS after discontinuation of natalizumab therapy. METHODS: This study is a longitudinal and serial cross-sectional assessment, in which 23 patients who were treated with natalizumab in the context of two phase III clinical trials were originally enrolled. A subgroup of patients was followed over 14 months. The annual relapse rate, neurologic disease progression assessed by the Expanded Disability Status Scale, disease surrogate markers on MRI, cellular and humoral immune markers in peripheral blood and CSF, and adverse events of the drug were monitored. RESULTS: With regard to clinical disease activity, neuroimaging, and immune responses, the majority of patients in our cohort were stable. Decreased lymphocyte cell numbers and altered cell ratios returned to normal 14 months after cessation of natalizumab. No infectious complications were observed. CONCLUSION: This is the first long-term follow-up of patients who discontinued natalizumab. We did not observe a clinical, radiographic, or immunologic rebound phenomenon after discontinuation of natalizumab therapy.

AB - OBJECTIVE: Natalizumab is a humanized recombinant monoclonal antibody against very late activation antigen-4 approved for the treatment of patients with multiple sclerosis (MS). A phase II study failed to demonstrate a difference between natalizumab treatment groups and the placebo group with regard to gadolinium enhancing lesions on MRI 3 months after discontinuation of therapy. The objective of this study was to assess clinical MS disease activity, surrogate disease markers on MRI, immunologic parameters in peripheral blood and CSF, as well as safety in patients with MS after discontinuation of natalizumab therapy. METHODS: This study is a longitudinal and serial cross-sectional assessment, in which 23 patients who were treated with natalizumab in the context of two phase III clinical trials were originally enrolled. A subgroup of patients was followed over 14 months. The annual relapse rate, neurologic disease progression assessed by the Expanded Disability Status Scale, disease surrogate markers on MRI, cellular and humoral immune markers in peripheral blood and CSF, and adverse events of the drug were monitored. RESULTS: With regard to clinical disease activity, neuroimaging, and immune responses, the majority of patients in our cohort were stable. Decreased lymphocyte cell numbers and altered cell ratios returned to normal 14 months after cessation of natalizumab. No infectious complications were observed. CONCLUSION: This is the first long-term follow-up of patients who discontinued natalizumab. We did not observe a clinical, radiographic, or immunologic rebound phenomenon after discontinuation of natalizumab therapy.

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Immunologic, clinical, and radiologic status 14 months after cessation of natalizumab therapy

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