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Carla Olivares, M. Sc. , Analía Ricci, M. Sc. , Mariela Bilotas, Ph. D

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Presentation on theme: "Carla Olivares, M. Sc. , Analía Ricci, M. Sc. , Mariela Bilotas, Ph. D"— Presentation transcript:

1 The inhibitory effect of celecoxib and rosiglitazone on experimental endometriosis 
Carla Olivares, M.Sc., Analía Ricci, M.Sc., Mariela Bilotas, Ph.D., Rosa Inés Barañao, Ph.D., Gabriela Meresman, Ph.D.  Fertility and Sterility  Volume 96, Issue 2, Pages (August 2011) DOI: /j.fertnstert Copyright © 2011 American Society for Reproductive Medicine Terms and Conditions

2 Figure 1 Effect of celecoxib and rosiglitazone on endometriotic-like lesion establishment and growth. Mice underwent surgery for endometriosis induction. After 28 days of treatment with vehicle, celecoxib, rosiglitazone, or both drugs simultaneously, the mice were sacrificed, and the number of lesions established was counted and measured. (A) Celecoxib and the combined treatment (Cele + Rosi) statistically significantly reduced the mean number of lesions established per mouse. (B) Celecoxib and rosiglitazone, separately, and the combined therapy (Cele + Rosi) statistically significantly reduced implant size. Results are expressed as mean ± standard error of the mean. ∗P<.05 versus control group. ∗∗∗P<.001 versus control group. n = 11 (control), 12 (celecoxib), 8 (rosiglitazone), 10 (Cele + Rosi). Fertility and Sterility  , DOI: ( /j.fertnstert ) Copyright © 2011 American Society for Reproductive Medicine Terms and Conditions

3 Figure 2 Effect of celecoxib and rosiglitazone on endometriotic-like lesion epithelial cell proliferation. Mice underwent surgery for endometriosis induction. After 28 days of treatment with vehicle, celecoxib, rosiglitazone, or both drugs simultaneously, the mice were sacrificed, and the implants were removed and fixed. Cell proliferation within the implants was evaluated by immunohistochemistry of proliferating cell nuclear antigen (PCNA). (A) After treatment with celecoxib, rosiglitazone, or both drugs simultaneously (Cele + Rosi), epithelial cell proliferation was statistically significantly diminished compared with control mice. Results are expressed as mean ± standard error of the mean. ∗∗P<.01 versus control group; ∗∗∗P<.001 versus control group. (B) Representative photographs of PCNA staining. Control group (i), celecoxib group (ii), rosiglitazone group (iii), celecoxib + rosiglitazone group (iv). Inset: negative control, an immunoglobulin of the same immunoglobulin class and concentration as the primary antibody was used. Magnification ×400. n = 8 (control), 7 (celecoxib), 5 (rosiglitazone), 5 (Cele + Rosi). Fertility and Sterility  , DOI: ( /j.fertnstert ) Copyright © 2011 American Society for Reproductive Medicine Terms and Conditions

4 Figure 3 Effect of celecoxib and rosiglitazone on endometriotic-like lesion epithelial cell apoptosis. Mice underwent surgery for endometriosis induction. After 28 days of treatment with vehicle, celecoxib, rosiglitazone, or both drugs simultaneously, the mice were sacrificed, and the implants were removed and fixed. Apoptosis within the implants was evaluated by TUNEL assay. (A) After treatment with celecoxib, rosiglitazone, or both drugs simultaneously (Cele + Rosi), epithelial cell apoptosis was enhanced compared with the control group. Results are expressed as mean ± standard error of the mean. ∗P<.05 versus control group. (B) Representative photographs of TUNEL staining. Control group (i), celecoxib group (ii), rosiglitazone group (iii), celecoxib + rosiglitazone group (iv). Inset: negative control, sections were incubated in absence of TdT. Magnification ×400. n = 6 (control), 7 (celecoxib), 5 (rosiglitazone), 5 (Cele + Rosi). Fertility and Sterility  , DOI: ( /j.fertnstert ) Copyright © 2011 American Society for Reproductive Medicine Terms and Conditions

5 Figure 4 Effect of celecoxib and rosiglitazone on endometriotic-like lesion vascular density. Mice underwent surgery for endometriosis induction. After 28 days of treatment with vehicle, celecoxib, rosiglitazone, or both drugs simultaneously, the mice were sacrificed, and the implants were removed and fixed. Vascular density within the implants was evaluated by performing immunohistochemical analysis of CD31 and CD34. (A) CD31: After treatment with rosiglitazone and both drugs simultaneously (Cele + Rosi), the vascular density was diminished compared with control mice. (B) CD34: After treatment with celecoxib, rosiglitazone, or both drugs simultaneously (Cele + Rosi), the vascular density was diminished compared with control mice. Results are expressed as mean ± standard error of the mean. ∗P<.05 versus control group; ∗∗P<.01 versus control group. n = 5 (control), 5 (celecoxib), 5 (rosiglitazone), 5 (Cele + Rosi). Fertility and Sterility  , DOI: ( /j.fertnstert ) Copyright © 2011 American Society for Reproductive Medicine Terms and Conditions

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