TY - JOUR
T1 - Collection of hematopoietic stem cells from patients with autoimmune diseases
AU - Burt, R. K.
AU - Fassas, A.
AU - Snowden, J. A.
AU - Van Laar, J. M.
AU - Kozak, T.
AU - Wulffraat, N. M.
AU - Nash, R. A.
AU - Dunbar, C. E.
AU - Arnold, R.
AU - Prentice, G.
AU - Bingham, S.
AU - Marmont, A. M.
AU - McSweeney, P. A.
N1 - Funding Information:
1Northwestern University Medical Center, Department of Medicine, Chicago, IL, USA; 2George Papanicolaou General Hospital, Department of Hematology, Thessaloniki, Greece; 3University Hospital of Leicester, Leicester, UK; 4St Vincent’s Hospital, Sydney, Australia; 5Leiden University Medical Center, Leiden, The Netherlands; 6University Hospital Kralovske Vinohrady, Prague, Czech Republic; 7Universitair Medisch Centrum, Utrecht, The Netherlands; 8Fred Hutchinson Research Cancer Center, Seattle, WA, USA; 9National Institutes of Health, National Heart Lung and Blood Institute, Hematology Branch, Bethesda, MD, USA; 10Universitatsklinikum Campus Charite Mitte, Berlin, Germany; 11Royal Free and University Medical School, London, UK; 12Leeds General Infirmary, Leeds, UK; 13Centro Trapianti di Midollo Osseo, Ospedale San Martino, Genoa, Italy; and 14University of Colorado, Denver, CO, USA
Funding Information:
Transplantation Unit, Ospedale Civile, Pescara, Italy; Willem E Fibbe, Leiden University Medical Center, Leiden, The Netherlands; Richard D Huhn, Coriell Institute for Medical Research, Camden, New Jersey, USA; Andres Theil and Oliver Rosen, Universitatsklini-kum Campus Charite Mitte, Berlin, Germany; Ann Traynor, Kehuan Luo, Borko Jovanovicv and Yu Oyama, Northwestern University Medical Center, Department of Medicine, Chicago, Illinois, USA; Laura Herbert, Royal Free and University Medical School, London, UK; Susan Leitman, National Institutes of Health, Warren Grant Magnuson Clinical Center, Bethesda, Maryland, USA; Keith Sullivan, Duke University Medical Center, Durham, North Carolina, USA; Ineke Slaper, Universitair Medisch Centrum, Utrecht, The Netherlands.
PY - 2001
Y1 - 2001
N2 - We reviewed data from 24 transplant centers in Asia, Australia, Europe, and North America to determine the outcomes of stem cell collection including methods used, cell yields, effects on disease activity, and complications in patients with autoimmune diseases. Twenty-one unprimed bone marrow harvests and 174 peripheral blood stem cell mobilizations were performed on 187 patients. Disease indications were multiple sclerosis (76 patients), rheumatoid arthritis (37 patients), scleroderma (26 patients), systemic lupus erythematosus (19 patients), juvenile chronic arthritis (13 patients), idiopathic autoimmune thrombocytopenia (8 patients), Behcet's disease (3 patients), undifferentiated vasculitis (3 patients), polychondritis (1 patient) and polymyositis (1 patient). Bone marrow harvests were used in the Peoples Republic of China and preferred worldwide for children. PBSC mobilization was the preferred technique for adult stem cell collection in America, Australia, and Europe. Methods of PBSC mobilization included G-CSF (5, 10, or 16 μg/kg/day) or cyclophosphamide (2 or 4 g/m2) with either G-CSF (5 or 10 μg/kg/day) or GM-CSF (5 μg/kg/day). Bone marrow harvests were without complications and did not affect disease activity. A combination of cyclophosphamide and G-CSF was more likely to ameliorate disease activity than G-CSF alone (P < 0.001). G-CSF alone was more likely to cause disease exacerbation than the combination of cyclophosphamide and G-CSF (P = 0.003). Three patients died as a result of cyclophosphamide-based stem cell collection (2.6% of patients mobilized with cyclophosphamide). When corrected for patient weight and apheresis volume, progenitor cell yields tended to vary by underlying disease, prior medication history and mobilization regimen. Trends in the approaches to, and results of, progenitor cell mobilization are suggested by this survey. While cytokine-based mobilization appears less toxic, it is more likely to result in disease reactivation. Optimization with regard to cell yields and safety are likely to be disease-specific and prospective disease-specific studies of mobilization procedures appear warranted.
AB - We reviewed data from 24 transplant centers in Asia, Australia, Europe, and North America to determine the outcomes of stem cell collection including methods used, cell yields, effects on disease activity, and complications in patients with autoimmune diseases. Twenty-one unprimed bone marrow harvests and 174 peripheral blood stem cell mobilizations were performed on 187 patients. Disease indications were multiple sclerosis (76 patients), rheumatoid arthritis (37 patients), scleroderma (26 patients), systemic lupus erythematosus (19 patients), juvenile chronic arthritis (13 patients), idiopathic autoimmune thrombocytopenia (8 patients), Behcet's disease (3 patients), undifferentiated vasculitis (3 patients), polychondritis (1 patient) and polymyositis (1 patient). Bone marrow harvests were used in the Peoples Republic of China and preferred worldwide for children. PBSC mobilization was the preferred technique for adult stem cell collection in America, Australia, and Europe. Methods of PBSC mobilization included G-CSF (5, 10, or 16 μg/kg/day) or cyclophosphamide (2 or 4 g/m2) with either G-CSF (5 or 10 μg/kg/day) or GM-CSF (5 μg/kg/day). Bone marrow harvests were without complications and did not affect disease activity. A combination of cyclophosphamide and G-CSF was more likely to ameliorate disease activity than G-CSF alone (P < 0.001). G-CSF alone was more likely to cause disease exacerbation than the combination of cyclophosphamide and G-CSF (P = 0.003). Three patients died as a result of cyclophosphamide-based stem cell collection (2.6% of patients mobilized with cyclophosphamide). When corrected for patient weight and apheresis volume, progenitor cell yields tended to vary by underlying disease, prior medication history and mobilization regimen. Trends in the approaches to, and results of, progenitor cell mobilization are suggested by this survey. While cytokine-based mobilization appears less toxic, it is more likely to result in disease reactivation. Optimization with regard to cell yields and safety are likely to be disease-specific and prospective disease-specific studies of mobilization procedures appear warranted.
KW - Autoimmune disease
KW - Hematopoietic stem cell transplantation
KW - Mobilization
UR - http://www.scopus.com/inward/record.url?scp=0034894424&partnerID=8YFLogxK
UR - http://www.scopus.com/inward/citedby.url?scp=0034894424&partnerID=8YFLogxK
U2 - 10.1038/sj.bmt.1703081
DO - 10.1038/sj.bmt.1703081
M3 - Article
C2 - 11498738
AN - SCOPUS:0034894424
SN - 0268-3369
VL - 28
SP - 1
EP - 12
JO - Bone Marrow Transplantation
JF - Bone Marrow Transplantation
IS - 1
ER -