Synergistic antitumor activity of pro‐apoptotic agent <scp><scp>PAC‐1</scp></scp> with cisplatinum by the activation of <scp><scp>CASP3</scp></scp> in pulmonary adenocarcinoma cell line H1299

Huang, Jinlong; Liang, Haibin; Zhang, Xuchao; Xie, Zhi; Jin, Tian-en

doi:10.1111/ajco.12419

Cited by 6 publications

(5 citation statements)

References 40 publications

(39 reference statements)

Supporting

Mentioning

Contrasting

Order By: Relevance

“…10 fold in H1299 cells and 3 fold in P31 cells when compared to the parental cells. These data are consistent with data for cisplatin sensitivity reported for H1299 cells by Johansson et al [ 15 ] and Huang et al [ 21 ], for H1299r cells [ 15 ] and for P31 and P31r cells reported by Janson et al [ 22 ] and Johansson et al [ 15 ]. In addition, we observed that there was a significantly greater proliferation rate in the sensitive cell lines when compared to the resistant cell lines for both H1299 and P31 cells, an observation consistent with that measured previously for these cells by Tyler et al [ 23 ].…”

Section: Discussionsupporting

confidence: 92%

Bioenergetics of acquired cisplatin resistant H1299 non-small cell lung cancer and P31 mesothelioma cells

et al. 2017

View full text Add to dashboard Cite

Acquired cisplatin resistance is a common feature of tumours following cancer treatment with cisplatin and also of non-small cell lung cancer (H1299) and mesothelioma (P31) cell lines exposed to cisplatin. To elucidate the cellular basis of acquired cisplatin resistance, a comprehensive bioenergetic analysis was undertaken. We demonstrate that cellular oxygen consumption was significantly decreased in cisplatin resistant cells and that the reduction was primarily due to reduced mitochondrial activity as a result of reduced mitochondrial abundance. The differential mitochondrial abundance was supported by data showing reduced sirtuin 1 (SIRT1), peroxisome-proliferator activator receptor-γ co-activator 1-alpha (PGC1α), sirtuin 3 (SIRT3) and mitochondrial transcription factor A (TFAM) protein expression in resistant cells. Consistent with these data we observed increased reactive oxygen species (ROS) production and increased hypoxia inducible factor 1-alpha (HIF1α) stabilization in cisplatin resistant cells when compared to cisplatin sensitive controls. We also observed an increase in AMP kinase subunit α2 (AMPKα2) transcripts and protein expression in resistant H1299 cells. mRNA expression was also reduced for cisplatin resistant H1299 cells in these genes, however the pattern was not consistent in resistant P31 cells. There was very little change in DNA methylation of these genes, suggesting that the cells are not stably reprogrammed epigenetically. Taken together, our data demonstrate reduced oxidative metabolism, reduced mitochondrial abundance, potential for increased glycolytic flux and increased ROS production in acquired cisplatin resistant cells. This suggests that the metabolic changes are a result of reduced SIRT3 expression and increased HIF-1α stabilization.

show abstract

Section: Discussionsupporting

confidence: 92%

Bioenergetics of acquired cisplatin resistant H1299 non-small cell lung cancer and P31 mesothelioma cells

et al. 2017

View full text Add to dashboard Cite

show abstract

“…S1A–C). Collectively these results demonstrate that, in addition to general cytotoxins and inhibitors against BRAF V600E (Botham et al, 2016; Huang et al, 2016; Peh et al, 2016; Razi et al, 2015), PAC-1 is able to broadly enhance the caspase-3 activity of kinase inhibitors targeted to EGFR T790M , EML4-ALK, and BCR-ABL.…”

Section: Resultsmentioning

confidence: 73%

Overcoming Resistance to Targeted Anticancer Therapies through Small-Molecule-Mediated MEK Degradation

Peh

Boudreau

Smith

et al. 2018

Cell Chemical Biology

View full text Add to dashboard Cite

The discovery of mutant or fusion kinases that drive oncogenesis, and the subsequent approval of specific inhibitors for these enzymes, has been instrumental in the management of some cancers. However, acquired resistance remains a significant problem in the clinic, limiting the long-term effectiveness of most of these drugs. Here we demonstrate a general strategy to overcome this resistance through drug-induced MEK cleavage (via direct procaspase-3 activation) combined with targeted kinase inhibition. This combination effect is shown to be general across diverse tumor histologies (melanoma, lung cancer, and leukemia) and driver mutations (mutant BRAF or EGFR, fusion kinases EML4-ALK and BCR-ABL). Caspase-3-mediated degradation of MEK kinases results in sustained pathway inhibition and substantially delayed or eliminated resistance in cancer cells in a manner far superior to combinations with MEK inhibitors. These data suggest the generality of drug-mediated MEK kinase cleavage as a therapeutic strategy to prevent resistance to targeted anticancer therapies.

show abstract

“…Given that NSCLC has not been associated with genetic alterations directly affecting H3K27 methylation, our finding may provide a rationale to encourage exploration of the potential of GSKJ4 as an anticancer agent against a wider range of cancers than previously thought. The NSCLC cell lines used in this study were A549 (poorly differentiated adenocarcinoma with mutated KRAS, wild-type (wt) TP53 and wt EGFR), H1299 (poorly differentiated adenocarcinoma with wt KRAS, homozygous deletion of TP53 and wt EGFR) and PC9 (well differentiated adenocarcinoma with wt KRAS, wt TP53 and mutated EGFR) (32)(33)(34)(35)(36)(37)(38). Although A549 appeared to be somewhat more sensitive than the other two, GSKJ4 quite effectively inhibited the growth of all three cell lines at 2 μM, a concentration that did not affect the growth of normal human fibroblasts, which may imply that GSKJ4 exerts its anticancer effect irrespective of the genetic status of the KRAS, TP53 and EGFR genes.…”

Section: Discussionmentioning

confidence: 99%

Impact of H3K27 Demethylase Inhibitor GSKJ4 on NSCLC Cells Alone and in Combination with Metformin

Watarai

Okada

Kuramoto

et al. 2016

View full text Add to dashboard Cite

show abstract

Synergistic antitumor activity of pro‐apoptotic agent PAC‐1 with cisplatinum by the activation of CASP3 in pulmonary adenocarcinoma cell line H1299

Cited by 6 publications

References 40 publications

Bioenergetics of acquired cisplatin resistant H1299 non-small cell lung cancer and P31 mesothelioma cells

Bioenergetics of acquired cisplatin resistant H1299 non-small cell lung cancer and P31 mesothelioma cells

Overcoming Resistance to Targeted Anticancer Therapies through Small-Molecule-Mediated MEK Degradation

Impact of H3K27 Demethylase Inhibitor GSKJ4 on NSCLC Cells Alone and in Combination with Metformin

Contact Info

Product

Resources

About