COMPARATIVE MOUSE MICRONUCLEUS EVALUATION IN BONE-MARROW AND SPLEEN USING IMMUNOFLUORESCENCE AND WRIGHTS GIEMSA

被引：7

作者：

KRISHNA, G

URDA, G

THEISS, JC

机构：

[1] Molecular Toxicology Section, Department of Pathology and Experimental Toxicology, Parke-Davis Pharmaceutical Research, Ann Arbor, MI 48105

来源：

MUTATION RESEARCH | 1994年 / 323卷 / 1-2期

关键词：

ANTIKINETOCHORE ANTIBODY TECHNIQUE; CLASTOGENICITY; ANEUGENICITY; MICRONUCLEUS ASSAY; (MOUSE); BONE MARROW; SPLEEN; CYCLOPHOSPHAMIDE; VINCRISTINE;

D O I：

10.1016/0165-7992(94)90039-6

中图分类号：

Q3 [遗传学];

学科分类号：

071007 ; 090102 ;

摘要：

Bone marrow and spleen toxicity, clastogenicity and aneugenicity were analyzed in the CD, mouse using an antikinetochore antibody(AKA) procedure (Krishna et al., Mutation Res., 282, 159-169, 1992). Further, to verify the fluorescence micronucleus (MN) analysis, additional slides were stained with Wright's Giemsa and results were compared. 5 mice per sex were treated with cyclophosphamide (CP) (40 mg/kg) or vincristine (VC) (0.1 or 0.2 mg/kg). Slides were prepared 24 h postdose using a column fractionation procedure. Per animal, 400 total erythrocytes (TEs) for toxicity and 2000 polychromatic erythrocytes (PCEs) for MN per tissue were analyzed. In the fluorescent method, the clastogen, CP, produced MNPCEs predominantly devoid of kinetochores (K) and the aneugen, VC, produced mostly MNPCEs containing K. The MNPCE frequency did not differ significantly between tissues; however, it differed statistically between sexes. On an overall basis, spleen had significantly lower PCE to TE ratios compared to bone marrow. In general, CP and VC caused a small, but statistically significant decrease in PCE frequencies compared to controls, suggesting possible toxicity to these tissues at the given doses. The data on Wright's stain indicated that the proportion of PCEs and MNPCEs in general, were comparable to those using fluorescent stain. This study further confirms the usefulness of an AKA-staining technique in a multiple genetic endpoint evaluation under a single set of microscopic conditions.

引用

页码：11 / 20

页数：10

共 50 条

[41] COMPARISON OF RESULTS FROM MOUSE BONE-MARROW CHROMOSOME ABERRATION AND MICRONUCLEUS TESTS
SHELBY, MD
WITT, KL
ENVIRONMENTAL AND MOLECULAR MUTAGENESIS, 1995, 25 (04) : 302 - 313
[42] BONE-MARROW MICRONUCLEUS ASSAY - A REVIEW OF THE MOUSE STOCKS USED AND THEIR PUBLISHED MEAN SPONTANEOUS MICRONUCLEUS FREQUENCIES
SALAMONE, MF
MAVOURNIN, KH
ENVIRONMENTAL AND MOLECULAR MUTAGENESIS, 1994, 23 (04) : 239 - 273
[43] SIMULATION STUDY OF THE EFFECTS OF MULTIPLE TREATMENTS IN THE MOUSE BONE-MARROW MICRONUCLEUS TEST
HAYASHI, M
SOFUNI, T
MORITA, T
MUTATION RESEARCH, 1991, 252 (03): : 281 - 287
[44] ACTIVITY OF 1,4-DIOXANE IN MOUSE BONE-MARROW MICRONUCLEUS ASSAYS
TINWELL, H
ASHBY, J
MUTATION RESEARCH-GENETIC TOXICOLOGY, 1994, 322 (02): : 148 - 150
[45] KINETICS OF MICRONUCLEUS FORMATION IN RELATION TO CHROMOSOMAL-ABERRATIONS IN MOUSE BONE-MARROW
HAYASHI, M
SOFUNI, T
ISHIDATE, M
MUTATION RESEARCH, 1984, 127 (02): : 129 - 137
[46] RESULTS OF MOUSE BONE-MARROW MICRONUCLEUS STUDIES ON 1,4-DIOXANE
MCFEE, AF
ABBOTT, MG
GULATI, DK
SHELBY, MD
MUTATION RESEARCH-GENETIC TOXICOLOGY, 1994, 322 (02): : 145 - 148
[47] Methylphenidate is not clastogenic in cultured human lymphocytes and in the mouse bone-marrow micronucleus test
Suter, Willi
Martus, HansJoerg
Elhajouji, Azeddine
MUTATION RESEARCH-GENETIC TOXICOLOGY AND ENVIRONMENTAL MUTAGENESIS, 2006, 607 (02) : 153 - 159
[48] MULTIPLE DOSING EFFECTS OF BENZO[A]PYRENE IN THE MOUSE BONE-MARROW MICRONUCLEUS TEST
SHIMADA, H
SATAKE, S
ITOH, S
HATTORI, C
HAYASHI, M
ISHIDATE, M
MUTATION RESEARCH, 1991, 252 (01): : 107 - 107
[49] INFLUENCE OF VEGETABLE OIL VEHICLES ON BONE-MARROW PROLIFERATION IN THE MOUSE MICRONUCLEUS TEST
SIMULA, AP
PRIESTLY, BG
MUTATION RESEARCH, 1991, 261 (01): : 83 - 84
[50] SUSPECTED SPINDLE POISONS ANALYZED BY MICRONUCLEUS TEST USING MOUSE BONE-MARROW AND HUMAN-LYMPHOCYTES
VANHUMMELEN, P
MUTATION RESEARCH, 1990, 234 (06): : 386 - 386

← 1 2 3 4 5 →