Claims
- 1. A transgenic mouse homozygous for Hox11 gene inactivation, wherein the Hox11 gene is inactivated by insertion of a heterologous nucleic acid sequence into the Hox11 gene via homologous recombination, wherein the inactivation of the Hox11 gene prevents expression of the Hox11 gene, and whereby the mouse is asplenic.
- 2. A transgenic mouse having integrated into its genome the human Hox11 gene operably linked to a promoter specifically active in thymocytes,
- wherein expression of the Hox11 gene in the thymus cells of the transgenic mouse renders the thymus of the transgenic mouse smaller than the thymus of mice not expressing the human Hox11 gene.
- 3. The transgenic mouse of claim 2 wherein T cells of the transgenic mouse exhibit a developmental block at the CD4.sup.- 8.sup.- to CD4.sup.+ 8.sup.+ transition.
- 4. The transgenic mouse of claim 2 wherein the thymus of the transgenic mouse is dysplastic.
- 5. The transgenic mouse of claim 2 wherein the total number of thymocytes in the thymus of the transgenic mouse is less than 50% of the total number of thymocytes in the thymus of mice not expressing the human Hox11 gene.
- 6. The transgenic mouse of claim 2 wherein the total number of T cells in the spleen and lymph nodes of the transgenic mouse is less than the total number of T cells in the spleen and lymph nodes mice not expressing the human Hox11 gene.
- 7. The transgenic mouse of claim 2 wherein thymocytes cultured from the transgenic mouse die more rapidly than thymocytes cultured from mice not expressing the human Hox11 gene.
- 8. The transgenic mouse of claim 2 wherein thymocytes of the transgenic mouse exhibit neoplasia.
- 9. A method for screening for a compound, wherein the compound affects a developmental and/or pathological condition due to expression of the human Hox11 gene in the thymus or T cells that do not normally express the human Hox11 gene, the method comprising:
- administering the compound to the transgenic mouse of claim 2, and
- monitoring the mouse for a change in the developmental and/or pathological condition.
- 10. The method of claim 9 wherein the developmental and/or pathological condition is the production of dysplastic T cells, and wherein the transgenic mouse is monitored for a change in the production of dysplastic T cells.
- 11. The method of claim 9 wherein the developmental and/or pathological condition is the production of neoplastic T cells, and wherein the transgenic mouse is monitored for a change in the production of neoplastic T cells.
- 12. The method of claim 9 wherein the developmental and/or pathological condition is that the total number of thymocytes in the thymus of the transgenic mouse is less than 50% of the total number of thymocytes in the thymus of mice not expressing the human Hox11 gene, and wherein the transgenic mouse is monitored for a change in the total number of thymocytes in the thymus of the transgenic mouse.
- 13. The method of claim 9 wherein the developmental and/or pathological condition is that the total number of T cells in the spleen and lymph nodes of the transgenic mouse is less than the total number of T cells in the spleen and lymph nodes mice not expressing the human Hox11 gene, and wherein the transgenic mouse is monitored for a change in the total number of T cells in the spleen and lymph nodes of the transgenic mouse.
Parent Case Info
This is a continuation of application Ser. No. 08/231,728 filed on Apr. 20, 1994, now abandoned.
US Referenced Citations (2)
Number |
Name |
Date |
Kind |
4868116 |
Morgan et al. |
Sep 1989 |
|
4980286 |
Morgan et al. |
Dec 1990 |
|
Foreign Referenced Citations (1)
Number |
Date |
Country |
WO 9301286 |
Jan 1993 |
WOX |
Continuations (1)
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Number |
Date |
Country |
Parent |
231728 |
Apr 1994 |
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