Lysosome‐dependent <scp>FOXA1</scp> ubiquitination contributes to luminal lineage of advanced prostate cancer

Celada, Sherly I.; Li, Guoliang; Celada, Lindsay J.; Lu, Wenfu; Kanagasabai, Thanigaivelan; Feng, Weiran; Cao, Zhen; Salsabeel, Nazifa; Mao, Ninghui; Brown, LaKendria K.; Mark, Zaniya A.; Izban, Michael G.; Ballard, Billy R.; Zhou, Xinchun; Adunyah, Samuel E.; Matusik, Robert J.; Wang, Xiaofei; Chen, Zhenbang

doi:10.1002/1878-0261.13497

Cited by 5 publications

(2 citation statements)

References 68 publications

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“…13 2.2 | SKP2 knockdown (KD) cells with short hairpin RNA and KDM5B knockout (KO) cells with CRISPR/Cas9 C4-2B SKP2 KD and PC3 SKP2 KD cells were generated as previously described. 17 Briefly, 293FT cells were transfected with plasmids carrying SKP2-shRNA or scrambled sequence, along with psPAX2 and pMD2.G envelope plasmids in Lipofectamine 2000 (ThermoFisher Scientific). The viral supernatant was collected 48 h posttransfection and filtered using a 0.45 μm filter.…”

Section: Cell Culturementioning

confidence: 99%

Co‐targeting SKP2 and KDM5B inhibits prostate cancer progression by abrogating AKT signaling with induction of senescence and apoptosis

Brown,

Kanagasabai,

et al. 2024

The Prostate

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BackgroundProstate cancer (PCa) is the second‐leading cause of cancer mortalities in the United States and is the most commonly diagnosed malignancy in men. While androgen deprivation therapy (ADT) is the first‐line treatment option to initial responses, most PCa patients invariably develop castration‐resistant PCa (CRPC). Therefore, novel and effective treatment strategies are needed. The goal of this study was to evaluate the anticancer effects of the combination of two small molecule inhibitors, SZL‐P1‐41 (SKP2 inhibitor) and PBIT (KDM5B inhibitor), on PCa suppression and to delineate the underlying molecular mechanisms.MethodsHuman CRPC cell lines, C4‐2B and PC3 cells, were treated with small molecular inhibitors alone or in combination, to assess effects on cell proliferation, migration, senescence, and apoptosis.ResultsSKP2 and KDM5B showed an inverse regulation at the translational level in PCa cells. Cells deficient in SKP2 showed an increase in KDM5B protein level, compared to that in cells expressing SKP2. By contrast, cells deficient in KDM5B showed an increase in SKP2 protein level, compared to that in cells with KDM5B intact. The stability of SKP2 protein was prolonged in KDM5B depleted cells as measured by cycloheximide chase assay. Cells deficient in KDM5B were more vulnerable to SKP2 inhibition, showing a twofold greater reduction in proliferation compared to cells with KDM5B intact (p < 0.05). More importantly, combined inhibition of KDM5B and SKP2 significantly decreased proliferation and migration of PCa cells as compared to untreated controls (p < 0.005). Mechanistically, combined inhibition of KDM5B and SKP2 in PCa cells abrogated AKT activation, resulting in an induction of both cellular senescence and apoptosis, which was measured via Western blot analysis and senescence‐associated β‐galactosidase (SA‐β‐Gal) staining.ConclusionsCombined inhibition of KDM5B and SKP2 was more effective at inhibiting proliferation and migration of CRPC cells, and this regimen would be an ideal therapeutic approach of controlling CRPC malignancy.

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Section: Cell Culturementioning

confidence: 99%

Co‐targeting SKP2 and KDM5B inhibits prostate cancer progression by abrogating AKT signaling with induction of senescence and apoptosis

Brown,

Kanagasabai,

et al. 2024

The Prostate

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“…Del Giudice et al [112] highlighted the role of FOXA1 in rewiring the alternative splicing landscape in prostate cancer, involving chromatin access, regulation of splicing factors, and alternative splicing of exons influencing patient survival. Celada et al [113] discovered that lysosome-dependent FOXA1 ubiquitination contributes to the luminal lineage of advanced prostate cancer. Therefore, FOXA1 plays a significant role in the occurrence and progression of prostate cancer, directly influencing the development of prostate cancer through the regulation of AR, and can also exert its effects through other pathways that do not affect AR expression levels.…”

Section: Other Roles Of Foxa1 In Prostate Cancermentioning

confidence: 99%

The Role of FOXA1 in Human Normal Development and Its Functions in Sex Hormone-Related Cancers

Zhu,

Wei,

Deng

et al. 2024

Front. Biosci. (Landmark Ed)

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The ubiquitin-proteasome system in the regulation of tumor dormancy and recurrence

Alhasan,

Morozov,

Guzhova

et al. 2024

Biochimica et Biophysica Acta (BBA) - Reviews on Cancer

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Lysosome‐dependent FOXA1 ubiquitination contributes to luminal lineage of advanced prostate cancer

Cited by 5 publications

References 68 publications

Co‐targeting SKP2 and KDM5B inhibits prostate cancer progression by abrogating AKT signaling with induction of senescence and apoptosis

Co‐targeting SKP2 and KDM5B inhibits prostate cancer progression by abrogating AKT signaling with induction of senescence and apoptosis

The Role of FOXA1 in Human Normal Development and Its Functions in Sex Hormone-Related Cancers

The ubiquitin-proteasome system in the regulation of tumor dormancy and recurrence

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