Targeted Inhibition of the KLF6 Splice Variant, KLF6 SV1, Suppresses Prostate Cancer Cell Growth and Spread

Narla, Goutham; DiFeo, Analisa; Shen, Yao; Banno, Asoka; Hod, Eldad A.; Reeves, Helen L.; Qu, Rui; Camacho-Vanegas, Olga; Levine, Alice C.; Kirschenbaum, Alexander; Chan, Andrew M.; Friedman, Scott L.; Martignetti, John A.

doi:10.1158/0008-5472.can-05-0217

Cited by 149 publications

(161 citation statements)

References 33 publications

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“…It is associated with increased production of three alternatively spliced, dominant-negative KLF6 isoforms. Whereas full-length KLF6 has a role in tumour suppression, the alternatively spliced KLF6 isoforms seem to have oncogenic functions, as specific disruption of these variants suppressed rather than enhanced tumorigenesis 68 . The dominantnegative properties of these splice variants are illustrated by their abilities to counteract induction of CDKN1A and proliferative arrest by full-length KLF6 (REF.…”

Section: Klf4 As An Oncogenementioning

confidence: 99%

KLF4, p21 and context-dependent opposing forces in cancer

2005

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| Krüppel-like factors are transcriptional regulators that influence several cellular functions, including proliferation. Recent studies have shown that one family member, KLF4, can function both as a tumour suppressor and an oncogene. The ability of KLF4 to affect the levels of expression of the cell-cycle regulator p21 seems to be involved, in that this protein might function as a switch that determines the outcome of KLF4 signalling. Is this role of p21 restricted to KLF4, or does p21 represent a nodal point for signals from multiple other factors with opposing functions in cancer?

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Section: Klf4 As An Oncogenementioning

confidence: 99%

KLF4, p21 and context-dependent opposing forces in cancer

2005

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“…To date, three alternatively spliced KLF6 isoforms, KLF6-SV1, -SV2 and -SV3, have been identified [21]. KLF6-SV1 is an oncogenic splice variant of KLF6, and increased KLF6-SV1 expression is associated with poor prognosis in prostate, lung, and ovarian cancers [10,13,[21][22][23]. Furthermore, KLF6-SV1 has been shown to be biologically active, antagonizing the tumor suppressor function of KLF6 and promoting tumor growth and dissemination in both ovarian and prostate cancer models [20,21,23].…”

Section: Introductionmentioning

confidence: 99%

“…KLF6-SV1 is an oncogenic splice variant of KLF6, and increased KLF6-SV1 expression is associated with poor prognosis in prostate, lung, and ovarian cancers [10,13,[21][22][23]. Furthermore, KLF6-SV1 has been shown to be biologically active, antagonizing the tumor suppressor function of KLF6 and promoting tumor growth and dissemination in both ovarian and prostate cancer models [20,21,23]. Evidence from many cancer types and different stages of tumorigenesis and progression has confirmed important roles for KLF6 and KLF6-SV1; in particular, that the overexpression of KLF6-SV1 is associated with metastatic potential and with decreased survival and that small interfering RNA (siRNA)-mediated downregulation of KLF6-SV1 decreases tumor growth in vitro [20,21] and in vivo [10,23].…”

Section: Introductionmentioning

confidence: 99%

“…Furthermore, KLF6-SV1 has been shown to be biologically active, antagonizing the tumor suppressor function of KLF6 and promoting tumor growth and dissemination in both ovarian and prostate cancer models [20,21,23]. Evidence from many cancer types and different stages of tumorigenesis and progression has confirmed important roles for KLF6 and KLF6-SV1; in particular, that the overexpression of KLF6-SV1 is associated with metastatic potential and with decreased survival and that small interfering RNA (siRNA)-mediated downregulation of KLF6-SV1 decreases tumor growth in vitro [20,21] and in vivo [10,23]. In addition, KLF6-SV1 has been identified as a novel anti-apoptotic protein, independent of a tumor cell's p53 status [10,24], which suggested its potential as a novel target for anti-cancer therapy.…”

Section: Introductionmentioning

confidence: 99%

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A small interfering RNA targeting the KLF6 splice variant, KLF6-SV1, as gene therapy for gastric cancer

Chen

Sun

et al. 2011

Gastric Cancer

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Background Accumulating evidence suggests that the tumor suppressor gene Kruppel-like factor 6 (KLF6) and its dominant-negative splice form KLF6-SV1 play important roles in both the development and progression of cancer. However, the role of KLF6-SV1 in gastric cancer remains largely unknown. Methods KLF6-SV1 expression was detected in various human gastric cancer cell lines and gastric cancer patient samples by reverse transcriptase polymerase chain reaction (RT-PCR) and Western blotting. Small interfering RNA (siRNA) was used to inhibit KLF6-SV1 expression in BGC-823 and SGC-7901 cell lines. The effects of downregulation of KLF6-SV1 by siRNA on cell proliferation, migration, invasion, and tumor growth were examined in vitro and in vivo.

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“…Polyclonal pools of each short interfering RNA (siRNA)-infected cell line were collected and the levels of KLF6 and KLF6-SV1 were determined by qRT-PCR and Western blot. RNA isolation, reverse transcription and quantification was performed as previously described (Narla et al, 2005b) using E-cadherin-forward: 5 0 -CAA AGT GGG CAC AGA TGG TGT G-3 0 and reverse: 5 0 -CTG CTT GGA TTC CAG AAA CGG-3 0 and GAPDH forward: 5 0 -CAA TGA CCC CTT CAT TGA CC-3 0 and glyceraldehyde-3-phosphate dehydrogenase (GAPDH) reverse: 5 0 -GAT CTC GCT CCT GGA AGA TG-3 0 primers. Expression levels were calculated by normalizing each cDNA to GAPDH and then using this normalized value to calculate fold change.…”

mentioning

confidence: 99%

E-cadherin is a novel transcriptional target of the KLF6 tumor suppressor

et al. 2006

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The tumor suppressor KLF6 is a member of the Kru¨ppel-like family of transcription factors, which has been implicated in the pathogenesis of several human carcinomas. Uncovering the transcriptional targets relevant for its tumorigenic properties, including cellular proliferation and invasion, will be essential to understanding possible mechanisms by which KLF6 and its antagonistic splice form, KLF6-SV1, regulate this development. To begin defining possible metastatic-related pathways, we analysed the effect of KLF6 dysregulation on a recognized suppressor of cellular invasion, E-cadherin. Targeted KLF6 reduction in an ovarian cancer cell line, SKOV-3, resulted in a 50% reduction of E-cadherin expression (Po0.01) and conversely, KLF6-SV1 silencing upregulated E-cadherin approximately fivefold (Po0.0001). These changes resulted from KLF6 directly transactivating the E-cadherin promoter as demonstrated by luciferase promoter assay and chromatin immunoprecipitation (ChIP). KLF6-mediated changes in E-cadherin levels were accompanied by downstream changes in both the subcellular localization of b-catenin and c-myc expression levels. Moreover, and consistent with these experimental findings, patient-derived epithelial ovarian tumors with low KLF6 and high KLF6-SV1 expression ratios had significantly decreased E-cadherin expression (Po0.0001). These combined findings highlight the E-cadherin pathway as a novel and functionally important mediator by which changes in KLF6 and KLF6-SV1 can directly alter ovarian tumor invasion and metastasis.

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Targeted Inhibition of the KLF6 Splice Variant, KLF6 SV1, Suppresses Prostate Cancer Cell Growth and Spread

Cited by 149 publications

References 33 publications

KLF4, p21 and context-dependent opposing forces in cancer

KLF4, p21 and context-dependent opposing forces in cancer

A small interfering RNA targeting the KLF6 splice variant, KLF6-SV1, as gene therapy for gastric cancer

E-cadherin is a novel transcriptional target of the KLF6 tumor suppressor

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