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1. Heightened susceptibility to chronic gastritis, hyperplasia and metaplasia in Kcnq1 mutant mice.

2. Etoposide induces heritable chromosomal aberrations and aneuploidy during male meiosis in the mouse.

3. Alterations in the reproductive patterns of female mice exposed to xenobiotics.

4. Induced mouse chromosomal rearrangements as tools for identifying critical developmental genes and pathways.

5. Dominant lethal mutations, heritable translocations, and unscheduled DNA synthesis induced in male mouse germ cells by glycidamide, a metabolite of acrylamide.

7. Exposure to ethylene oxide during the early zygotic period induces skeletal anomalies in mouse fetuses.

8. Dominant lethal and heritable translocation tests with chlorambucil and melphalan in male mice.

9. Limb and lower-body duplications induced by retinoic acid in mice.

10. The rodent dominant-lethal assay.

11. Cytogenetic analysis of malformed mouse fetuses derived from balanced translocation heterozygotes.

12. A new frontier in understanding the mechanisms of developmental abnormalities.

13. Developmental anomalies derived from exposure of zygotes and first-cleavage embryos to mutagens.

14. Bleomycin: female-specific dominant lethal effects in mice.

15. Acrylamide: dermal exposure produces genetic damage in male mouse germ cells.

16. Developmental response of zygotes exposed to similar mutagens.

17. Mouse dominant lethal and bone marrow micronucleus studies on methyl vinyl sulfone and divinyl sulfone.

18. Comparison of two stocks of mice in spermatogonial response to different conditions of radiation exposure.

19. RPE dysplasia with retinal duplication in a mutant mouse strain.

20. Induction of specific-locus mutations in male germ cells of the mouse by acrylamide monomer.

21. Female-specific mutagenic response of mice to hycanthone.

22. Female-specific dominant lethal effects in mice.

23. Molecular and genetic characterization of a radiation-induced structural rearrangement in mouse chromosome 2 causing mutations at the limb deformity and agouti loci.

24. Increased incidence of developmental anomalies among descendants of carriers of methylenebisacrylamide-induced balanced reciprocal translocations.

25. Concentration-response curves for ethylene-oxide-induced heritable translocations and dominant lethal mutations.

26. Review of the mutagenicity of ethylene oxide.

27. Mouse models for understanding human developmental anomalies.

29. A report of the U.S. Environmental Protection Agency Gene-Tox Program. Evaluation of mutagenicity assays for purposes of genetic risk assessment.

30. Exposure of female mice to ethylene oxide within hours after mating leads to fetal malformation and death.

33. Pseudo dominant-lethal response in female mice treated with plant oils.

34. Genetic lesions induced by chemicals in spermatozoa and spermatids of mice are repaired in the egg.

36. Mouse germ cell mutation tests in genetic risk evaluation of chemical mutagens.

37. Response of mouse spermatogonial stem cells to X-ray induction of heritable reciprocal translocations.

38. Heritable translocation test in mice.

39. Chromosome malsegregation and embryonic lethality induced by treatment of normally ovulated mouse oocytes with nocodazole.

41. Ethanol-induced late fetal death in mice exposed around the time of fertilization.

42. Heritable translocation and dominant-lethal mutation induction with ethylene oxide in mice.

43. Dominant lethal effects of acrylamide in male mice.

44. Timing of sperm penetration, pronuclear formation, pronuclear DNA synthesis, and first cleavage in naturally ovulated mouse eggs.

45. 239Plutonium-induced heritable translocations in male mice.

47. Difference between two hybrid stocks of mice in the incidence of congenital abnormalities following X-ray exposure of stem-cell spermatogonia.

48. Difference in the ratio of dominant-lethal mutations to heritable translocations produced in mouse spermatids and fully mature sperm after treatment with triethylenemelamine (TEM).

50. Mutagen-induced fetal anomalies and death following treatment of females within hours after mating.

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