Inhibition of DHHC20-Mediated EGFR Palmitoylation Creates a Dependence on EGFR Signaling

Runkle, Kristin B.; Kharbanda, Akriti; Stypulkowski, Ewa; Cao, Xing Jun; Wang, Wei; Garcia, Benjamin A.; Witze, Eric S.

doi:10.1016/j.molcel.2016.04.003

Cited by 168 publications

(194 citation statements)

References 20 publications

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“…DHHC20 is also known to be expressed in MDA-MB-231 cells, where it palmitoylates EGFR and attenuates EGFR signaling (28). We asked whether loss of DHHC20 would affect protein localization.…”

Section: Resultsmentioning

confidence: 99%

The depalmitoylase APT1 directs the asymmetric partitioning of Notch and Wnt signaling during cell division

2018

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Asymmetric cell division results in two distinctly fated daughter cells. A molecular hallmark of asymmetric division is the unequal partitioning of cell fate determinants. We have previously established that growth factor signaling promotes protein depalmitoylation to foster polarized protein localization, which in turns drives migration and metastasis. Here, we report protein palmitoylation as a key mechanism for the asymmetric partitioning of the cell fate determinants Numb and β-catenin through the activity of the depalmitoylating enzyme APT1. Using point mutations, we show specific palmitoylated residues on Numb are required for asymmetric localization. By live-cell imaging, we show that reciprocal interactions between APT1 and the Rho-family GTPase CDC42 promote the asymmetric localization of Numb and β-catenin to the plasma membrane. This in turn restricts Notch- and Wnt-responsive transcriptional activity to one daughter cell. Moreover, we show altering APT1 expression changes the transcriptional signatures of MDA-MB-231 triple receptor–negative breast cancer cells similarly to changes in Notch and β-catenin–mediated Wnt signaling. We also show that loss of APT1 depletes a specific subpopulation of tumorigenic cells in colony formation assays. Together, our findings demonstrate that APT1-mediated depalmitoylation is a major mechanism of asymmetric cell division maintaining Notch and Wnt-associated protein dynamics, gene expression, and cellular functions.

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Section: Resultsmentioning

confidence: 99%

The depalmitoylase APT1 directs the asymmetric partitioning of Notch and Wnt signaling during cell division

2018

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“…1A) (16). Although inhibition of DHHC20 by shRNA leads to an increase in sensitivity to gefitinib-induced cell death, it is still unclear if this effect was directly mediated by inhibiting EGFR palmitoylation or if it is the effect of another unknown target of DHHC20.…”

Section: Resultsmentioning

confidence: 99%

“…Although inhibition of DHHC20 by shRNA leads to an increase in sensitivity to gefitinib-induced cell death, it is still unclear if this effect was directly mediated by inhibiting EGFR palmitoylation or if it is the effect of another unknown target of DHHC20. We previously showed that EGFR is palmitoylated on the C-terminal tail and that mutating one of the palmitoylated cysteine residues 1025 to alanine is sufficient to reduce receptor palmitoylation, induce receptor autophosphorylation, adaptor binding and downstream signaling to AKT and ERK when transiently expressed in NIH3T3 cells (16). To test if blocking EGFR palmitoylation directly increases gefitinib sensitivity of human cancer cells, we developed a conditional system for expressing wild type EGFR (EGFR WT ) or palmitoylation defective EGFR with cysteine 1025 mutated to alanine (EGFR C1025A ) in MDA-MB-231 cells with a tetracycline-inducible promoter.…”

Section: Resultsmentioning

confidence: 99%

“…DHHC20 palmitoylates the epidermal growth factor receptor (EGFR) on specific cysteine residues on the C-terminal tail, suppressing its activation. Unexpectedly, inhibition of DHHC20 in both breast and lung cancer cells increases induction of cell death in response to the EGFR inhibitor gefitinib, despite the fact the cells harbor activated Kras mutations and wild type EGFR (16). Mutations in Kras, predominantly an amino acid substitution at codon 12 or 13, lead to upregulation of the Ras/MAPK signaling and ERK activation, ultimately driving cell division.…”

Section: Introductionmentioning

confidence: 99%

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Induced sensitivity to EGFR inhibitors is mediated by palmitoylated cysteine 1025 of EGFR and requires oncogenic Kras

Kharbanda

Runkle

Wang

et al. 2017

Biochemical and Biophysical Research Communications

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Currently, there are no effective therapeutic strategies targeting Kras driven cancers, and therefore, identifying new targeted therapies and overcoming drug resistance have become paramount for effective long-term cancer therapy. We have found that reducing expression of the palmitoyl transferase DHHC20 increases cell death induced by the EGFR inhibitor gefitinib in Kras and EGFR mutant cell lines, but not MCF7 cells harboring wildtype Kras. We show that the increased gefitinib sensitivity in cancer cells induced by DHHC20 inhibition is mediated directly through loss of palmitoylation on a previously identified cysteine residue in the C-terminal tail of EGFR. We utilized an EGFR point mutant in which the palmitoylated cysteine 1025 is mutated to alanine (EGFRC1025A), that results in receptor activation. Expression of the EGFR mutant alone in NIH3T3 cells does not increase sensitivity to gefitinib-induced cell death. However, when EGFRC1025A is expressed in cells expressing activated KrasG12V, EGFR inhibitor induced cell death is increased. Surprisingly, lung cancer cells harboring the EGFR inhibitor resistant mutation, T790M, become sensitive to EGFR inhibitor treatment when DHHC20 is inhibited. Finally, the small molecule, 2-bromopalmitate, which has been shown to inhibit palmitoyl transferases, acts synergistically with gefitinib to induce cell death in the gefitinib resistant cell line NCI-H1975.

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“…DHHC proteins and their substrates play important roles in tumorigenesis (13,14). Palmitoylation of H-and N-Ras facilitates Ras localization to the plasma membrane and is required for protein activity (15,16), and inhibiting ZDHHC20 palmitoyltransferase leads to the dependence of cancer cells on EGF receptor signaling for survival (17).…”

Section: Introductionmentioning

confidence: 99%

EZH2 Palmitoylation Mediated by ZDHHC5 in p53-Mutant Glioma Drives Malignant Development and Progression

Chen

Wang

et al. 2017

Cancer Research

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Gliomas with mutant p53 occurring in 30% of glioma patients exhibit therapeutic resistance and poor outcomes. In this study, we identify a novel mechanism through which mutant p53 drives cancer cell survival and malignant growth. We documented overexpression of the zinc finger protein ZDHHC5 in glioma compared with normal brain tissue and that this event tightly correlated with p53 mutations. Mechanistic investigations revealed that mutant p53 transcriptionally upregulated ZDHHC5 along with the nuclear transcription factor NF-Y. These events contributed to the development of glioma by promoting the self-renewal capacity and tumorigenicity of glioma stem-like cells, by altering the palmitoylation and phosphorylation status of the tumor suppressor EZH2. Taken together, our work highlighted ZDHHC5 as a candidate therapeutic target for management of p53-mutated gliomas.

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Inhibition of DHHC20-Mediated EGFR Palmitoylation Creates a Dependence on EGFR Signaling

Cited by 168 publications

References 20 publications

The depalmitoylase APT1 directs the asymmetric partitioning of Notch and Wnt signaling during cell division

The depalmitoylase APT1 directs the asymmetric partitioning of Notch and Wnt signaling during cell division

Induced sensitivity to EGFR inhibitors is mediated by palmitoylated cysteine 1025 of EGFR and requires oncogenic Kras

EZH2 Palmitoylation Mediated by ZDHHC5 in p53-Mutant Glioma Drives Malignant Development and Progression

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