Thymidine kinase obliteration: creation of transgenic mice with controlled immune deficiency

  1. R A Heyman,
  2. E Borrelli,
  3. J Lesley,
  4. D Anderson,
  5. D D Richman,
  6. S M Baird,
  7. R Hyman, and
  8. R M Evans
  1. Howard Hughes Medical Institute, San Diego, CA 92138.

Abstract

The cell-specific expression of herpes simplex virus 1 thymidine kinase (HSV-1-tk) has provided a simple and highly efficient technique to achieve conditional ablation of targeted cell types in transgenic mice. The ablation is induced by treating transgenic animals expressing HSV-1-tk with the antiherpetic drug ganciclovir. In lymphoid tissues of mice expressing HSV-1-tk from an immunoglobulin promoter, administration of ganciclovir leads to massive destruction of B- and T-cell lineages. Tissues not expressing HSV-1-tk are insensitive to drug treatment. After depletion of greater than 99% of total thymocytes, a number of progenitor cells remain that are able to repopulate all T-cell lineages within 7 days. The ability to control and direct ablation allows for creation of conditional mutant phenotypes at precise periods of development. This technique also provides a potential means to enrich stem cell populations as well as permitting the creation of animal models for particular pathological conditions.

« Previous | Next Article »Table of Contents

This Article

  1. PNAS April 1, 1989 vol. 86 no. 8 2698-2702
  1. » Abstract
  2. Full Text (PDF)

Classifications

About Our New Site Design >>
Link: Advanced Search

This Week's Issue

  1. November 18, 2008, 105 (46)
  1. Current Issue
  1. Alert me to new issues of PNAS

Most