A Role for the Mitogen-activated Protein Kinase Kinase Kinase 1 in Epithelial Wound Healing

Deng, Maoxian; Chen, Wei-Li; Takatori, Atsushi; Peng, Zhimin; Zhang, Lin; Mongan, Maureen; Parthasarathy, R.; Sartor, Maureen A.; Miller, Marian L.; Yang, Jianhua; Su, Bing; Kao, Winston W.‐Y.; Xia, Ying

doi:10.1091/mbc.e06-02-0102

Cited by 67 publications

(66 citation statements)

References 39 publications

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“…MEKK3 knockout is embryo lethal, displaying inadequate fetal-maternal vascularization (Yang et al, 2000), whereas loss of MEKK4 activity is largely perinatal lethal, and is associated with defective neural tube closure . In contrast, both MEKK1 and MEKK2 are developmentally dispensable, with recent evidence suggesting that losses of these proteins are associated with impaired tissue remodeling associated with wound healing and homeostasis Yamashita et al, 2005;Deng et al, 2006). These models indicate that, while other MKKKs also regulate activation of these MAPK modules, the MEKKs each control one or more cellular functions that are not redundant and thus not compensated for by other MKKKs.…”

Section: Mekk Groupmentioning

confidence: 99%

Role of mitogen-activated protein kinase kinase kinases in signal integration

2007

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Mitogen-activated protein kinases (MAPKs) are members of a dynamic protein kinase network through which diverse stimuli regulate the spatio-temporal activities of complex biological systems. MAPKs regulate critical cellular functions required for homeostasis such as the expression of cytokines and proteases, cell cycle progression, cell adherence, motility and metabolism. MAPKs therefore influence cell proliferation, differentiation, survival, apoptosis and development. In vertebrates, five MAPK families are regulated by MAPK kinase kinase-MAPK kinase-MAPK (MKKK-MKK-MAPK) phosphorelay systems. There are at least 20 MKKKs that selectively phosphorylate and activate different combinations of the seven MKKs, resulting in a specific activation profile of members within the five MAPK families. MKKKs are differentially activated by upstream stimuli including cytokines, antigens, toxins and stress insults providing a mechanism to integrate the activation of different MAPKs with the cellular response to each stimulus. Thus, MKKKs can be considered as 'signaling hubs' that regulate the specificity of MAPK activation. In this review, we describe how the MKKK 'hub' function regulates the specificity of MAPK activation, highlighting MKKKs as targets for therapeutic intervention in cancer and other diseases.

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Section: Mekk Groupmentioning

confidence: 99%

Role of mitogen-activated protein kinase kinase kinases in signal integration

2007

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“…Adenoviruses containing cDNA for an N-terminal hemagglutin (HA)-tagged human MEKK1 [MEKK1(WT)] or for HA-MEKK1(KM), a ATPbinding site mutant, were described elsewhere (Deng et al, 2006). The plasmids for Exp-MEKK1, HA-JNK1 and HA-JNK2 were described previously (Xia et al, 1998) and the plasmids for HA-JNK1(CTN) and HA-JNK2 (GTS) containing site-specific mutations at amino acids 177 and 179 sites were generated using a QuikChange site-directed mutagenesis kit (Stratagene).…”

Section: Mice Reagents and Antibodiesmentioning

confidence: 99%

Differential transmission of MEKK1 morphogenetic signals by JNK1 and JNK2

et al. 2008

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*JNK1 and JNK2 are two ubiquitously expressed isoforms that exert redundant roles in many physiological processes, but the extent of their relative contributions to these processes has not been well characterized. We show that both JNK isoforms transmit MEK kinase 1 (MEKK1)-mediated morphogenetic signals during mouse embryonic eyelid closure. However, JNK1 and JNK2 are not synonymous, because MEKK1 is haploinsufficient for normal eyelid closure in Jnk1-null mice, but is haplosufficient in Jnk2-null mice. In the Mekk1 heterozygous background, a more efficient phosphorylation of JNK1 than JNK2 leads to differential downstream reactions, such as c-Jun phosphorylation and PAI1 expression in the developing eyelid epithelium. Differences in efficiency of phosphorylation are attributed to JNK1 Gly177 and Ser179 -residues that are absent in JNK2 -which promote a less ordered structural conformation. This leads to more favorable JNK phosphorylation by activin B morphogenetic signals mediated by the MEKK1-MKK4 pathway. Interestingly, Mekk1-Jnk1-Jnk2 triple hemizygotes display a partial eye-open phenotype at birth, suggesting that all three genes dose-dependently contribute to morphogenetic eyelid closure. We propose that a MEKK1-JNK1/2 axis governs the JNK activation levels to control downstream transcriptional events and eyelid morphogenesis and that reduction of upstream MEKK1 signals uncovers analogous but differential roles of JNK1 and JNK2 in a biological process.

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“…Therefore, the epithelium in eyelids moved very slowly. There was no significant difference in cell migration ability, as determined using a wound-healing assay, between adult wild-type and MEKK1 -/-mice exhibiting the EOB phenotype (Deng et al, 2006). It is likely that abundant subcutaneous cytokines may serve as an alternative pathway to promote wound healing.…”

Section: Gene Namementioning

confidence: 90%

“…The developing eyelids are composed of loose mesenchyme covered by an epithelial sheet, the epidermis (outer surface), and conjunctiva (inner surface), as well as the periderm, which covers the epidermis (Deng et al, 2006). Only the peridermal and epidermal layers are involved in eyelid fusion.…”

Section: Gene Namementioning

confidence: 99%