Abstract
Constitutive depletion of p21-activated kinase 4 (PAK4) in the mouse causes embryonic lethality associated with heart and brain defects. Given that conventional gene depletion of PAK1 or PAK3 caused functional deficits in the mouse pancreas, while gene depletion of PAK5 or PAK6 did not, we asked if PAK4 might have a functional role in pancreas development. We therefore introduced conditional, Pdx1-Cre-mediated, pancreatic PAK4 gene depletion in the mouse, verified by loss of PAK4 protein expression in the pancreas. PAK4 knock-out (KO) mice were born at Mendelian ratios in both genders. Further, morphological and immunohistochemical examinations and quantifications indicated that exocrine, endocrine and ductal compartments retained the normal proportions and distributions upon PAK4 gene depletion. In addition, body weight records and a glucose tolerance test revealed no differences between WT and PAK4 KO mice. Together, this suggests that PAK4 is dispensable for mouse pancreas development. This will facilitate future use of our Pdx1-Cre-driven conditional PAK4 KO mouse model for testing in vivo potential functions of PAK4 in pancreatic disease models such as for pancreatitis and different pancreatic cancer forms.
Highlights
P21-activited kinases (PAKs), comprising a Rho GTPase-regulated serine/threonine kinase family, have been extensively studied and are implicated in many cellular processes, including cytoskeletal organization, cell cycle and cell survival[1,2,3]
p21-activated kinase 4 (PAK4) is highly expressed throughout development as well as in several cancer forms and it is ubiquitously expressed at low levels in many adult tissues[15,16,17]
Pdx1-Cre-driven PAK4 KO mice were viable and fertile, exhibited normal body weight as well as normal exocrine, endocrine and ductal cell morphology and displayed normal glucose tolerance. These results suggest that PAK4 is not essential for mouse pancreas development
Summary
P21-activited kinases (PAKs), comprising a Rho GTPase-regulated serine/threonine kinase family, have been extensively studied and are implicated in many cellular processes, including cytoskeletal organization, cell cycle and cell survival[1,2,3]. PAK4 is essential during development, because PAK4 KO caused embryonic lethality in mouse as a consequence of heart defects and abnormalities in extra-embryonic tissues and the embryonic vasculature[5]. Pdx1-Cre-driven PAK4 KO mice were viable and fertile, exhibited normal body weight as well as normal exocrine, endocrine and ductal cell morphology and displayed normal glucose tolerance. These results suggest that PAK4 is not essential for mouse pancreas development. This mouse model may be used to test the potential in vivo functions of PAK4 in pancreas disease models, such as for pancreatitis and different pancreas cancer forms
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