Sequence and Chromosomal Context Effects on Variegated Expression of Keratin 5/lacZ Constructs in Stratified Epithelia of Transgenic Mice

Sequence and Chromosomal Context Effects on Variegated Expression of Keratin 5/lacZ Constructs in Stratified Epithelia of Transgenic Mice

Angel Ramírez^a, Eric Milot^b, Immaculada Ponsa^c, Camelia Marcos-Gutiérrez^d, Angustias Page^a, Mirentxu Santos^a, José Jorcano^a, and Miguel Vidal^d
^a Cell and Molecular Biology, Centro Investigaciones Medio Ambientales y Energeticas (CIEMAT), 28040 Madrid, Spain,
^b Department of Cell Biology, Medical Genetics Center, Erasmus University, 3000 DR Rotterdam, The Netherlands,
^c Departament de Biologia Cellular, Fisiologia i Immunologia, Facultat de Medicina, Universitat Autònoma de Barcelona, E-08193 Bellaterra, Spain
^d Department of Developmental and Cell Biology, Centro Investigaciones Biológicas, 28006 Madrid, Spain

Corresponding author: Miguel Vidal, Department of Developmental and Cell Biology, Centro de Investigaciones Biológicas, Velázquez 144, 28006 Madrid, Spain., mvidal{at}cib.csic.es (E-mail)

Communicating editor: S. HENIKOFF

The expression of transgene loci in mammals often occurs ina heterocellular fashion resulting in variegated patterns ofexpression. We have examined the effect of chromosomal integrationsite, copy number, and transcriptionally activating sequenceson the variegation of a keratin 5-lacZ (K5Z) construct in thestratified epithelia of transgenic mice. lacZ expression inthese mice is always mosaic, and the ß-gal activityper cell is usually higher in the lines with a higher proportionof expressing cells. Similar constructs, in which cDNAs wereexchanged by lacZ sequences, showed no variegation. Also, whena strongly active, nonvariegating construct was coinjected withK5Z, most transgenic lines showed an almost homogeneous lacZexpression. The comparison of transgene arrays of differentcopies inserted at the same locus (obtained by using a lox/Cresystem) showed that the reduction of copy number does not leadto an increase in the proportion of cells that express the transgene.Finally, in most of the variegating or nonexpressing lines thetransgenes were located both at intermediate positions and atperitelomeric regions in the long chromosome arms. These findingssuggest that the probability and efficiency of expression ofK5Z genes depend on both long range chromosomal influences andon sequences in the transgene array.

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