Influence of Timing of Administration of 5-fluorouracil to Donors on Bone Marrow Engraftment in Nonmyeloablated Hosts

Overview

Journal Int J Hematol

Specialty Hematology

Date 2001 Sep 4

PMID 11530810

Citations 1

Authors

L Dhondt

J Carlson

B Benoit

J Reilly

C Grimaldi

J Wuu

J F Lambert

M S Dooner

P J Quesenberry

Affiliations

Soon will be listed here.

Abstract

We evaluated the engraftment and the cell cycle status of marrow cells at various times after 5-fluorouracil (5-FU) administration. 5-FU (150 mg/kg) was given to donor male BALB/c mice at 1, 2, 6, or 12 days prior to marrow harvest. The donor cells were then assessed in host nonmyeloablated female mice. Bone marrow engraftment of marrow treated with 5-FU was evaluated and compared to marrow treated with diluent (phosphate-buffered saline) at 3 and 10 weeks after marrow infusion. Our data show a rapid induction of an engraftment defect 1 day after 5-FU, persistence of this defect through day 6, and a recovery by day 12. Experiments using hydroxyurea (which selectively kills cells in the S phase) to determine the cell cycle status indicated that cells that engrafted in post-5-FU marrow were noncycling at days 1, 2, and 12 but cycling at day 6. Post-5-FU bone marrow was also analyzed in vitro by colony assays and its cycling status determined by 3H-thymidine suicide assay. High-proliferative-potential colony-forming cells (HPP-CFCs) and low-proliferative-potential colony-forming cells (LPP-CFCs) decreased rapidly 1 day after 5-FU, with a nadir observed at day 6 for HPP-CFCs and day 2 for LPP-CFCs. By day 12, LPP-CFCs showed a total recovery, but HPP-CFCs were still defective. Significant numbers of HPP-CFCs were cycling, mostly at days 6 and 8 after 5-FU, whereas LPP-CFCs appeared quiescent except at day 2. These results emphasize the importance of timing if post-5-FU marrow is used for gene therapy or marrow transplantation.

Citing Articles

Multistage hematopoietic stem cell regulation in the mouse: A combined biological and mathematical approach.

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PMID: 34877482 PMC: 8627979. DOI: 10.1016/j.isci.2021.103399.

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