Abstract. To artificially activate embryos in somatic cell nuclear transfer (SCNT), chemical treatment with ionomycin has been used to induce transient levels of Ca 2+ and initiate reprogramming of embryos. Ca 2+ oscillation occurs naturally several times after fertilization (several times with 15-to 30-min intervals). This indicates how essential additional Ca 2+ influx is for successful reprogramming of embryos. Hence, in this report, the experimental design was aimed at improving the developmental efficiency of cloned embryos by repetitive Ca 2+ transients rather than the commonly used ionomycin treatment (4 min). To determine optimal Ca 2+ inflow conditions, we performed three different repetitive ionomycin (10 μM) treatments in reconstructed embryos: Group 1 (4-min ionomycin treatment, once), Group 2 (30-sec treatment, 4 times, 15-min intervals) and Group 3 (1-min treatment, 4 times, 15-min intervals). Pronuclear formation rates were checked to assess the effects of repetitive ionomycin treatment on reprogramming of cloned embryos. Cleavage rates were investigated on day 2, and the formation rates of blastocysts (BLs) were examined on day 7 to demonstrate the positive effect of repeated ionomycin treatment. In Group 3, a significant increase in BL formation was observed [47/200 (23.50%), 44/197 (22.33%) and 69/195 (35.38%) in Groups 1, 2 and 3, respectively]. Culturing embryos with different ionomycin treatments caused no significant difference among the groups in terms of the total cell number of BLs (164.3, 158.5 and 145.1, respectively). Additionally, expression of the anti-apoptotic Bcl-2 gene and MnSOD increased significantly in Group 3, whereas the expression of the pro-apoptotic Bax decreased statistically. In conclusion, the present study demonstrated that repeated ionomycin treatment is an improved activation method that can increase the developmental competence of SCNT embryos by decreasing the incidence of apoptosis. Key words: Apoptosis, Bovine embryos, Ca 2+ oscillation, SCNT (J. Reprod. Dev. 58: [132][133][134][135][136][137][138][139] 2012) C a 2+ oscillation is a universal signaling cue that activates numerous cellular responses. Ca 2+ signaling is ubiquitous in some somatic cells and germ lines. In particular, in early embryo development, the fluctuating Ca 2+ concentration is a factor that brings about serial developmental mechanisms [1]. After fertilization, matured oocytes arrested in the metaphase stage of the second meiotic division (MII) turn into zygotes with subsequent signaling events such as depolarization, Ca 2+ oscillation, cortical reaction and pronucleus formation [2,3]. The exit from MII resumption and the further processes for forthcoming development do not occur before the concentration of intracellular Ca 2+ is increased by sperm penetration. Sperm is the initial signal for Ca 2+ release mediated by IP 3 (inositol trisphosphate), protein tyrosine kinases and PLC gamma (PLC-ζ in mammals), followed by reorganization of Ca 2+ -releasing machinery to trigger subsequent s...