Genetics, Vol. 161, 195-204, May 2002, Copyright © 2002

A hobo Transgene That Encodes the P-Element Transposase in Drosophila melanogaster: Autoregulation and Cytotype Control of Transposase Activity

Michael J. Simmonsa, Kevin J. Haleya, Craig D. Grimesa, John D. Raymonda, and Jarad B. Niemia
a Department of Genetics, Cell Biology and Development, University of Minnesota, Saint Paul, Minnesota 55108-1095

Corresponding author: Michael J. Simmons, Cell Biology and Development, 250 BioScience Ctr., 1445 Gortner Ave., University of Minnesota, St. Paul, MN 55108-1095., simmo004{at}tc.umn.edu (E-mail)

Communicating editor: K. GOLIC

Drosophila were genetically transformed with a hobo transgene that contains a terminally truncated but otherwise complete P element fused to the promoter from the Drosophila hsp70 gene. Insertions of this H(hsp/CP) transgene on either of the major autosomes produced the P transposase in both the male and female germlines, but not in the soma. Heat-shock treatments significantly increased transposase activity in the female germline; in the male germline, these treatments had little effect. The transposase activity of two insertions of the H(hsp/CP) transgene was not significantly greater than their separate activities, and one insertion of this transgene reduced the transposase activity of P(ry+, {Delta}2-3)99B, a stable P transgene, in the germline as well as in the soma. These observations suggest that, through alternate splicing, the H(hsp/CP) transgene produces a repressor that feeds back negatively to regulate transposase expression or function in both the somatic and germline tissues. The H(hsp/CP) transgenes are able to induce gonadal dysgenesis when the transposase they encode has P-element targets to attack. However, this ability and the ability to induce P-element excisions are repressed by the P cytotype, a chromosomal/cytoplasmic state that regulates P elements in the germline.





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