TY - JOUR
T1 - Hepatic regeneration in peroxisome proliferator-activated receptor α-null mice after partial hepatectomy
AU - Rao, M. Sambasiva
AU - Peters, Jeffrey M.
AU - Gonzalez, Frank J.
AU - Reddy, Janardan K.
N1 - Funding Information:
This research was supported by grants CA84472 (M.S.R) and GM23750 (J.K.R) from the National Institute of Health.
PY - 2002
Y1 - 2002
N2 - Peroxisome proliferator activated receptor α (PPARα), a member of the nuclear hormone receptor superfamily, is essential for hepatic pleiotropic effects induced by peroxisome proliferators including cell proliferation. In a previous study, we have shown that PPARα null mice do not show increased hepatocyte proliferation after administration of peroxisome proliferators, confirming that PPARα is necessary for peroxisome proliferator-induced cell proliferation. However, the role of PPARα, if any, in compensatory liver cell hyperplasia is not known. Therefore, we examined the role of PPARα in modulating compensatory liver cell proliferation occurring after partial hepatectomy (PH). Replicative DNA synthesis, as measured by bromodeoxyuridine labeling of liver cell nuclei, was significantly higher after 48 h post-hepatectomy in both wild type and PPARα-null mouse livers, as compared to sham-operated control mice. Interestingly, in PPARα-null mice labeling index was significantly higher at 60 h after hepatectomy compared to wild-type mice; however, at 72 and 84 h the values were comparable in both the groups. Hepatic levels of mRNAs encoding CDK1, CDK2, CDK4, cyclin B1, cyclin D1 and PCNA were all elevated at 60 and 72 h post-hepatectomy and this effect was similar in both PPARα genotypes. Similarly, CDK2, CDK4, cyclin B1, cyclin D1 and PCNA proteins also showed comparable increase in both the groups. These results show that PPARα receptor is not essential for increased expression of CDKs, cyclins, PCNA and enhanced cell proliferation that occur after PH. This strongly suggests that the signaling for increased cell proliferation in response to PH is distinctly different from that observed after administration of peroxisome proliferators.
AB - Peroxisome proliferator activated receptor α (PPARα), a member of the nuclear hormone receptor superfamily, is essential for hepatic pleiotropic effects induced by peroxisome proliferators including cell proliferation. In a previous study, we have shown that PPARα null mice do not show increased hepatocyte proliferation after administration of peroxisome proliferators, confirming that PPARα is necessary for peroxisome proliferator-induced cell proliferation. However, the role of PPARα, if any, in compensatory liver cell hyperplasia is not known. Therefore, we examined the role of PPARα in modulating compensatory liver cell proliferation occurring after partial hepatectomy (PH). Replicative DNA synthesis, as measured by bromodeoxyuridine labeling of liver cell nuclei, was significantly higher after 48 h post-hepatectomy in both wild type and PPARα-null mouse livers, as compared to sham-operated control mice. Interestingly, in PPARα-null mice labeling index was significantly higher at 60 h after hepatectomy compared to wild-type mice; however, at 72 and 84 h the values were comparable in both the groups. Hepatic levels of mRNAs encoding CDK1, CDK2, CDK4, cyclin B1, cyclin D1 and PCNA were all elevated at 60 and 72 h post-hepatectomy and this effect was similar in both PPARα genotypes. Similarly, CDK2, CDK4, cyclin B1, cyclin D1 and PCNA proteins also showed comparable increase in both the groups. These results show that PPARα receptor is not essential for increased expression of CDKs, cyclins, PCNA and enhanced cell proliferation that occur after PH. This strongly suggests that the signaling for increased cell proliferation in response to PH is distinctly different from that observed after administration of peroxisome proliferators.
KW - Bromodeoxyuridine
KW - Liver regeneration
KW - Partial hepatectomy
KW - Peroxisome proliferator-activated receptors
KW - Peroxisome proliferators
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U2 - 10.1016/S1386-6346(01)00119-X
DO - 10.1016/S1386-6346(01)00119-X
M3 - Article
AN - SCOPUS:0036120125
SN - 1386-6346
VL - 22
SP - 52
EP - 57
JO - Hepatology Research
JF - Hepatology Research
IS - 1
ER -