TGFbeta induces apoptosis and EMT in primary mouse hepatocytes independently of <it>p53</it>, <it>p21</it>^Cip1or <it>Rb </it>status

• Main Authors: Harrison David J, Harland Stephen N, Bellamy Christopher O, Sheahan Sharon, Prost Sandrine
• Format: Article
• Language: English
• Published: BMC 2008-07-01
• Series: BMC Cancer
• Online Access: http://www.biomedcentral.com/1471-2407/8/191

<p>Abstract</p> <p>Background</p> <p>TGFβ has pleiotropic effects that range from regulation of proliferation and apoptosis to morphological changes and epithelial-mesenchymal transition (EMT). Some evidence suggests that these effects may be interconnected. We have recently reported that P53, P21^Cip1and pRB, three critical regulators of the G1/S transition are variably involved in TGFβ-induced cell cycle arrest in hepatocytes. As these proteins are also involved in the regulation of apoptosis in many circumstances, we investigated their contribution to other relevant TGFβ-induced effects, namely apoptosis and EMT, and examined how the various processes were interrelated.</p> <p>Methods</p> <p>Primary mouse hepatocytes deficient in <it>p53, p21 </it>and/or <it>Rb</it>, singly or in combination were treated with TGFβ for 24 to 96 hours. Apoptosis was quantified according to morphology and by immunostaining for cleaved-capsase 3. Epithelial and mesenchymal marker expression was studied using immunocytochemistry and real time PCR.</p> <p>Results</p> <p>We found that TGFβ similarly induced morphological changes regardless of genotype and independently of proliferation index or sensitivity to inhibition of proliferation by TGFβ. Morphological changes were accompanied by decrease in E-cadherin and increased Snail expression but the mesenchymal markers (N-cadherin, SMAα and Vimentin) studied remained unchanged. TGFβ induced high levels of apoptosis in <it>p53-/-</it>, <it>Rb-/-</it>, <it>p21</it>^{<it>cip1</it>}-/- and control hepatocytes although with slight differences in kinetics. This was unrelated to proliferation or changes in morphology and loss of cell-cell adhesion. However, hepatocytes deficient in both <it>p53 </it>and <it>p21</it>^{<it>cip1</it>}were less sensitive to TGFβ-induced apoptosis.</p> <p>Conclusion</p> <p>Although <it>p53</it>, <it>p21</it>^Cip1and <it>pRb </it>are well known regulators of both proliferation and apoptosis in response to a multitude of stresses, we conclude that they are critical for TGFβ-driven inhibition of hepatocytes proliferation, but only slightly modulate TGFβ-induced apoptosis. This effect may depend on other parameters such as proliferation and the presence of other regulatory proteins as suggested by the consequences of <it>p53</it>, <it>p21</it>^Cip1double deficiency. Similarly, <it>p53</it>, <it>p21</it>^Cip1and <it>pRB </it>deficiency had no effect on the morphological changes and loss of cell adhesion which is thought to be critical for metastasis. This indicates that possible association of these genes with metastasis potential would be unlikely to involve TGFβ-induced EMT.</p>