Autologous hematopoietic cell transplantation following high-dose immunosuppressive therapy for advanced multiple sclerosis: long-term results

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Abstract

The purpose of the study was to determine the long-term safety and effectiveness of high-dose immunosuppressive therapy (HDIT) followed by autologous hematopoietic cell transplantation (AHCT) in advanced multiple sclerosis (MS). Total body irradiation, cyclophosphamide, and antithymocyte globulin were followed by transplantation of autologous, CD34-selected peripheral blood stem cells (PBSC). Neurological examinations, brain MRIs and cerebrospinal fluid (CSF) for oligoclonal bands (OCB) were serially evaluated. Patients (n=26, mean EDSS=7.0, 17 secondary progressive, 8 primary progressive, 1 relapsing/remitting) were followed for a median of 48 months after HDIT followed by AHCT. The 72-month probability of worsening ≥ 1.0 EDSS point was 0.52 (95% CI, 0.30 to 0.75). Five patients had an EDSS at baseline of ≤ 6.0; four of these had not failed treatment at last study visit. OCB in CSF persisted with minor changes in the banding pattern. Four new or enhancing lesions were seen on MRI, all within 13 months of treatment. In this population with high baseline EDSS, a significant proportion of patients with advanced MS remained stable as long as 7 years after transplant. Non-inflammatory events may have contributed to neurological worsening after treatment. HDIT/AHCT may be more effective in patients with less advanced relapsing/remitting MS.

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Most cited references 39

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A topic that has received attention in both the statistical and medical literature is the estimation of the probability of failure for endpoints that are subject to competing risks. Despite this, it is not uncommon to see the complement of the Kaplan-Meier estimate used in this setting and interpreted as the probability of failure. If one desires an estimate that can be interpreted in this way, however, the cumulative incidence estimate is the appropriate tool to use in such situations. We believe the more commonly seen representations of the Kaplan-Meier estimate and the cumulative incidence estimate do not lend themselves to easy explanation and understanding of this interpretation. We present, therefore, a representation of each estimate in a manner not ordinarily seen, each representation utilizing the concept of censored observations being 'redistributed to the right.' We feel these allow a more intuitive understanding of each estimate and therefore an appreciation of why the Kaplan-Meier method is inappropriate for estimation purposes in the presence of competing risks, while the cumulative incidence estimate is appropriate.

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The relation between inflammation and neurodegeneration in multiple sclerosis brains

Josa M. Frischer, Stephan Bramow, Assunta Dal-Bianco … (2009)

Some recent studies suggest that in progressive multiple sclerosis, neurodegeneration may occur independently from inflammation. The aim of our study was to analyse the interdependence of inflammation, neurodegeneration and disease progression in various multiple sclerosis stages in relation to lesional activity and clinical course, with a particular focus on progressive multiple sclerosis. The study is based on detailed quantification of different inflammatory cells in relation to axonal injury in 67 multiple sclerosis autopsies from different disease stages and 28 controls without neurological disease or brain lesions. We found that pronounced inflammation in the brain is not only present in acute and relapsing multiple sclerosis but also in the secondary and primary progressive disease. T- and B-cell infiltrates correlated with the activity of demyelinating lesions, while plasma cell infiltrates were most pronounced in patients with secondary progressive multiple sclerosis (SPMS) and primary progressive multiple sclerosis (PPMS) and even persisted, when T- and B-cell infiltrates declined to levels seen in age matched controls. A highly significant association between inflammation and axonal injury was seen in the global multiple sclerosis population as well as in progressive multiple sclerosis alone. In older patients (median 76 years) with long-disease duration (median 372 months), inflammatory infiltrates declined to levels similar to those found in age-matched controls and the extent of axonal injury, too, was comparable with that in age-matched controls. Ongoing neurodegeneration in these patients, which exceeded the extent found in normal controls, could be attributed to confounding pathologies such as Alzheimer's or vascular disease. Our study suggests a close association between inflammation and neurodegeneration in all lesions and disease stages of multiple sclerosis. It further indicates that the disease processes of multiple sclerosis may die out in aged patients with long-standing disease.

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We describe a method for correlating the immunoglobulin (Ig) proteomes with the B cell transcriptomes in human fluid and tissue samples, using multiple sclerosis as a paradigm. Oligoclonal Ig bands and elevated numbers of clonally expanded B cells in the cerebrospinal fluid (CSF) are diagnostic hallmarks of multiple sclerosis. Here we compared the Ig transcriptomes of B cells with the corresponding Ig proteomes in CSF samples from four subjects with multiple sclerosis. We created individual Ig transcriptome databases that contained the subject-specific mutations introduced by V(D)J recombination and somatic hypermutation and then searched the CSF for corresponding characteristic peptides by mass spectrometry. In each sample, the Ig transcriptomes and proteomes strongly overlapped, showing that CSF B cells indeed produce the oligoclonal Ig bands. This approach can be applied to other organ-specific diagnostic fluid or tissue samples to compare the Ig transcripts of local B cells with the corresponding antibody proteomes of individual subjects.

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Author and article information

Journal

Journal ID (nlm-journal-id): 8702459

Journal ID (pubmed-jr-id): 2334

Journal ID (nlm-ta): Bone Marrow Transplant

Journal ID (iso-abbrev): Bone Marrow Transplant.

Title: Bone Marrow Transplantation

ISSN (Print): 0268-3369

ISSN (Electronic): 1476-5365

Publication date Nihms-submitted: 29 September 2011

Publication date (Electronic): 07 November 2011

Publication date (Print): July 2012

Publication date PMC-release: 01 January 2013

Volume: 47

Issue: 7

Pages: 946-951

Affiliations

[1 ]Swedish Neuroscience Institute, Seattle, WA; University of Washington, Seattle, WA

[2 ]Department of Rehabilitation Medicine, Seattle, WA

[3 ]Department of Neurology, Seattle, WA

[4 ]Department of Radiology, Seattle, WA

[5 ]Department of Medicine, Seattle, WA

[6 ]Fred Hutchinson Cancer Research Center, Seattle, WA

[7 ]Colorado Blood and Cancer Institute, Denver, CO

[8 ]National Cancer Institute, Bethesda, MD

[9 ]City of Hope, Duarte, CA

Author notes

Corresponding Author: Richard A. Nash, MD, D1-100 Clinical Research Division, Fred Hutchinson Cancer Research Center, 1100 Fairview Ave N, PO Box 19024, Seattle, WA 98109, Phone: 206-320-2200, Fax: 206-667-4978, rnash@ 123456fhcrc.org

Article

Manuscript ID: NIHMS326930

DOI: 10.1038/bmt.2011.208

PMC ID: 3276694

PubMed ID: 22056644

SO-VID: 7161a3e3-dbac-495a-a0b9-265caa6640d1

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History

Funding

Funded by: National Cancer Institute : NCI

Award ID: P30 CA015704-38 || CA

Funded by: National Heart, Lung, and Blood Institute : NHLBI

Award ID: P01 HL036444-30 || HL

Funded by: National Institute of Allergy and Infectious Diseases Extramural Activities : NIAID

Award ID: N01 AI005419 || AI

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