Prevalidation of a model for predicting acute neutropenia by colony forming unit granulocyte/macrophage (CFU-GM) assay

A Pessina; B Albella; J Bueren; P Brantom; S Casati; L Gribaldo; C Croera; G Gagliardi; P Foti; R Parchment; D Parent-Massin; Y Sibiril; R Van Den Heuvel

doi:10.1016/s0887-2333(01)00085-6

Prevalidation of a model for predicting acute neutropenia by colony forming unit granulocyte/macrophage (CFU-GM) assay

Toxicol In Vitro. 2001 Dec;15(6):729-40. doi: 10.1016/s0887-2333(01)00085-6.

Authors

A Pessina¹, B Albella, J Bueren, P Brantom, S Casati, L Gribaldo, C Croera, G Gagliardi, P Foti, R Parchment, D Parent-Massin, Y Sibiril, R Van Den Heuvel

Affiliation

¹ Institute of Microbiology, Via Pascal 36, 20133, Milan, Italy. pessinaa@mailserver.unimi.it

PMID: 11698175
DOI: 10.1016/s0887-2333(01)00085-6

Abstract

This report describes an international prevalidation study conducted to optimise the Standard Operating Procedure (SOP) for detecting myelosuppressive agents by CFU-GM assay and to study a model for predicting (by means of this in vitro hematopoietic assay) the acute xenobiotic exposure levels that cause maximum tolerated decreases in absolute neutrophil counts (ANC). In the first phase of the study (Protocol Refinement), two SOPs were assessed, by using two cell culture media (Test A, containing GM-CSF; and Test B, containing G-CSF, GM-CSF, IL-3, IL-6 and SCF), and the two tests were applied to cells from both human (bone marrow and umbilical cord blood) and mouse (bone marrow) CFU-GM. In the second phase (Protocol Transfer), the SOPs were transferred to four laboratories to verify the linearity of the assay response and its interlaboratory reproducibility. After a further phase (Protocol Performance), dedicated to a training set of six anticancer drugs (adriamycin, flavopindol, morpholino-doxorubicin, pyrazoloacridine, taxol and topotecan), a model for predicting neutropenia was verified. Results showed that the assay is linear under SOP conditions, and that the in vitro endpoints used by the clinical prediction model of neutropenia are highly reproducible within and between laboratories. Valid tests represented 95% of all tests attempted. The 90% inhibitory concentration values (IC(90)) from Test A and Test B accurately predicted the human maximum tolerated dose (MTD) for five of six and for four of six myelosuppressive anticancer drugs, respectively, that were selected as prototype xenobiotics. As expected, both tests failed to accurately predict the human MTD of a drug that is a likely protoxicant. It is concluded that Test A offers significant cost advantages compared to Test B, without any loss of performance or predictive accuracy. On the basis of these results, we proposed a formal Phase II validation study using the Test A SOP for 16-18 additional xenobiotics that represent the spectrum of haematotoxic potential.

Publication types

Research Support, Non-U.S. Gov't
Validation Study

MeSH terms

Acute Disease
Animals
Bone Marrow Cells
Cell Count
Colony-Forming Units Assay*
Dogs
Fetal Blood
Granulocytes / drug effects*
Granulocytes / pathology
Humans
Macrophages / drug effects*
Macrophages / pathology
Male
Mice
Mice, Inbred C57BL
Mice, Inbred DBA
Models, Biological
Neutropenia / chemically induced*
Neutropenia / pathology
Predictive Value of Tests
Rats
Rats, Inbred F344
Reproducibility of Results
Xenobiotics / toxicity*

Substances

Xenobiotics