Mapping of Atypical Protein Kinase C within the Nerve Growth Factor Signaling Cascade: Relationship to Differentiation and Survival of PC12 Cells

doi:10.1128/MCB.20.13.4494-4504.2000

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Molecular and Cellular Biology, July 2000, p. 4494-4504, Vol. 20, No. 13
0270-7306/00/$04.00+0
Copyright © 2000, American Society for Microbiology. All rights reserved.

Mapping of Atypical Protein Kinase C within the Nerve Growth Factor Signaling Cascade: Relationship to Differentiation and Survival of PC12 Cells

Marie W. Wooten,^* M. Lamar Seibenhener, Kimberly B. W. Neidigh, and Michel L. Vandenplas

Department of Biological Sciences, Program in Cell and Molecular Biosciences, Auburn University, Auburn, Alabama

Received 21 September 1999/Returned for modification 28 October 1999/Accepted 20 March 2000

The pathway by which atypical protein kinase C (aPKC) contributes to nerve growth factor (NGF) signaling is poorly understood.We previously reported that in PC12 cells NGF-induced activationof mitogen-activated protein kinase (MAPK) occurs independentlyof classical and nonclassical PKC isoforms, whereas aPKC isoformswere shown to be required for NGF-induced differentiation. NGF-inducedactivation of PKC- $iota$ was observed to be dependent on phosphatidylinositol3-kinase (PI3K) and led to coassociation of PKC- $iota$ with Ras andSrc. Expression of dominant negative mutants of either Src (DN2)or Ras (Asn-17) impaired activation of PKC- $iota$ by NGF. At the levelof Raf-1, neither PKC- $iota$ nor PI3 kinase was required for activation;however, PKC- $iota$ could weakly activate MEK. Inhibitors of PKC- $iota$ activity and PI3K had no effect on NGF-induced MAPK or p38 activationbut reduced NGF-stimulated c-Jun N-terminal kinase activity. Src,PI3K, and PKC- $iota$ were likewise required for NGF-induced NF- $kappa$ B activationand cell survival, whereas Ras was not required for either survivalor NF- $kappa$ B activation but was required for differentiation. IKKexisted as a complex with PKC- $iota$ , Src and I $kappa$ B. Consistent witha role for Src in regulating NF- $kappa$ B activation, an absence of Srcactivity impaired recruitment of PKC- $iota$ into an IKK complex andmarkedly impaired NGF-induced translocation of p65/NF- $kappa$ B to thenucleus. These findings reveal that in PC12 cells, aPKCs comprisea molecular switch to regulate differentiation and survival responsescoupled downstream to NF- $kappa$ B. On the basis of these findings, Srcemerges as a critical upstream regulator of both PKC- $iota$ and theNF- $kappa$ Bpathway.

^* Corresponding author. Mailing address: Department of Biological Sciences, 331 Funchess Hall, Auburn University, Auburn, AL36849. Phone: (334) 844-9245. Fax: (334) 844-9234. E-mail: mwwooten{at}ag.auburn.edu.

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