Human Platelet Lysate Can Replace Fetal Bovine Serum for Clinical-scale Expansion of Functional Mesenchymal Stromal Cells

Overview

Journal Transfusion

Specialty Hematology

Date 2007 Jul 28

PMID 17655588

Citations 177

Authors

Katharina Schallmoser

Christina Bartmann

Eva Rohde

Andreas Reinisch

Karl Kashofer

Elke Stadelmeyer

Camilla Drexler

Gerhard Lanzer

Werner Linkesch

Dirk Strunk

Affiliations

Soon will be listed here.

Abstract

Background: Human multipotent mesenchymal stromal cells (MSCs) are promising candidates for a growing spectrum of regenerative and immunomodulatory cellular therapies. Translation of auspicious experimental results into clinical applications has been limited by the dependence of MSC propagation from fetal bovine serum (FBS).

Study Design And Methods: The capacity of human platelet lysate (HPL) to replace FBS for clinical-scale MSC propagation was analyzed.

Results: HPL could be efficiently produced from buffy coats. Multiplex analyses allowed a distinct HPL growth factor profile to be delineated. With a previously established two-step clinical-scale procedure, HPL was reproducibly more efficient than FBS in supporting MSC outgrowth. With only 3 x 10(5) primary culture-derived MSCs, a mean of 4.36 x 10(8) HPL-MSCs (range, 3.01 x 10(8)-5.40 x 10(8)) was obtained within a single secondary 11- to 13-day culture step. Although morphologically distinct, HPL-MSCs and FBS-MSCs did not differ significantly in terms of immunophenotype, differentiation potential in vitro, and lack of tumorigenicity in nude mice in vivo.

Conclusions: Replacing FBS with HPL prevents bovine prion, viral, and zoonose contamination of the stem cell product. This new efficient FBS-free two-step procedure for clinical-scale MSC propagation may represent a major step toward challenging new stem cell therapies.

Citing Articles

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