Effects of celecoxib and L-NAME on apoptosis and cell cycle ofMCF-7 CD44+/CD24–/low subpopulation

Majdzadeh, Maryam; Aliebrahimi, Shima; Vatankhah, Melody; Ostad, Seyed Nasser

doi:10.3906/biy-1703-101

Cited by 8 publications

(6 citation statements)

References 21 publications

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“…MTT assay was employed to study the cytotoxic effect of free drug, blank nanocarriers, and drugloaded nanocarrier 111,112 . 10 4 cells of MCF-7 were cultured on each well of 96-well plates and were incubated for 24h.…”

Section: Cell Proliferation Assaymentioning

confidence: 99%

One Pot Doxorubicin Partitioning and Encapsulation on Silica Nanoparticle, Applying Aqueous Two Phase System for Preparation of pH-Responsive Nanocarriers

Baghbanbashi¹,

Pazuki²,

Khoee³

2021

Preprint

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Providing an efficient system for drug delivery and chemotherapy has always been an important issue. Modification of the surface of silica nanoparticles (SiO2) provides an opportunity for achieving stimulus-sensitive drug delivery system. Here, we have modified the surface of SiO2 using hydrogen bonding interactions by employing an aqueous two-phase system (ATPS) based on polyethylene glycol and lysine. This novel biocompatible ATPS provides an environment for simultaneous drug encapsulation, SiO2 modification, and drug partitioning in one pot. Addition of SiO2 to ATPS increased the partitioning of doxorubicin (DOX) as an anti-cancer drug from 47.92 in the absence of nanoparticles to 92.33 due to the interactions between drug and nanoparticles. The formation of nanoformulation and its characteristics were investigated applying microscopy, spectroscopy and thermal analysis. Drug release study demonstrated that DOX is loaded on nanoformulations efficiently with an encapsulation efficiency of 63.84% and shows lower release in physiological environment compared to the unmodified nanoparticles. While in acidic conditions of pH 5.5, significant increase was observed in the release profile. MTT assay on MCF-7 cancer cells confirmed that the nanoformulations were non-toxic and DOX-loaded nanocarrier showed anti-cancer behavior. These results indicate that the prepared nanoformulations are promising nanocarriers for controlled drug release purposes.

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Section: Cell Proliferation Assaymentioning

confidence: 99%

One Pot Doxorubicin Partitioning and Encapsulation on Silica Nanoparticle, Applying Aqueous Two Phase System for Preparation of pH-Responsive Nanocarriers

Baghbanbashi¹,

Pazuki²,

Khoee³

2021

Preprint

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“…IC50 was determined as being 12.2 mM in DU145 cells. Majdzadeh et al 27 studied the effect of L-NAME on MCF-7 breast cancer cells and their IC50 was between 10 mM and 20 mM in the MTT test. In their study, the viabilities of MCF-7 cells at 10, 20, and 40 mM of L-NAME were nearly 80%, 40%, and <20%, while in the current study, the viabilities of DU145 cells at 8, 16, and 32 mM of L-NAME were 68.4%, 33.3%, and 12%, respectively.…”

Section: Discussionmentioning

confidence: 99%

“…In our study, we detected a dose-dependent rise in apoptotic markers and also confirmed this result by morphological analysis. In literature, in the study of Majdzadeh et al, 27 L-NAME was suggested to partially lead to apoptosis and proposed to show its effect by another cell death mechanism. In our study, we found increase in CASP3, CYCY, and Bax immunostaining as well as apoptotic hallmarks morphologically.…”

Section: Discussionmentioning

confidence: 99%

The effects of L-NAME on DU145 human prostate cancer cell line: A cytotoxicity-based study

et al. 2019

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Of all cancer types, prostate cancer is the second most common one with an age-standardized incidence rate of 29.3 per 100,000 men worldwide. Nitric oxide (NO) is both a radical and versatile messenger molecule involved in many physiological activities. NO was documented to be highly secreted and utilized by cancer cells. N ω-nitro-L-arginine methyl ester (L-NAME) is utilized for inhibiting NO synthase. Its worst long-term side effect is reported to be hypertension, hence less cytotoxic than chemotherapeutic agents. Herein, we carried out a cytotoxicity study on how different doses of L-NAME affect DU145 human prostate cancer cells. First, toxic doses of L-NAME were determined. Then, while antioxidant capacity was determined by glutathione and total antioxidant status, oxidative stress was evaluated by quantifying malondialdehyde, NO, and total oxidant status levels. Inflammatory effects of L-NAME were investigated by measuring tumor necrosis factor- α and interleukin-6 (IL-6) levels. Apoptotic effects of L-NAME were evaluated by measuring cytochrome C somatic and caspase 3 levels and by staining Bax protein. Finally, morphological analysis was performed. IC50 of L-NAME against DU145 cells was 12.2 mM. In L-NAME-treated DU145 cells, a dose-dependent increase in oxidative stress, inflammatory, and apoptotic marker proteins and decrease in antioxidant capacity were observed. While at the moderate dose of L-NAME, apoptotic changes were commonly observed, at higher doses, vacuolated and swollen cells were also recorded. We believe that the present study will encourage future studies by providing insights about dose and effects of L-NAME.

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“…Several studies [ 33–36 ] evaluated the impact of celecoxib on various cancer cell lines to determine their sensitivity to celecoxib alone or in combination with other anticancer agents. For instance, El‐Awady et al [ 34 ] stated the concentration‐dependent effect of celecoxib on five cancer cell lines (HeLa, HCT116, HepG2, MCF‐7, and U251).…”

Section: Celecoxib As Anticancer Agentmentioning

confidence: 99%

Recent advances in the development of celecoxib analogs as anticancer agents: A review

Abdelhaleem

Kassab

El‐Nassan

et al. 2022

Archiv der Pharmazie

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Celecoxib is a nonsteroidal anti-inflammatory drug (NSAID) designed to be a selective cyclooxygenase-2 (COX-2) inhibitor. It was approved by the U.S. Food and Drug Administration for the treatment of inflammatory diseases such as osteoarthritis and rheumatoid arthritis. Additionally, celecoxib demonstrated potent antitumor and chemopreventive effects in vitro, in vivo, and in patients. The mechanism of celecoxib's chemopreventive effect is still not fully identified, but it is assumed to be multifactorial. Celecoxib's anticancer activity has been described both as independent of and dependent on its COX-2 inhibitory activity. The current review summarizes the recent advances published between 2000 and 2022 on the structure-based optimization of celecoxib to develop compounds with promising anticancer activity. The structure-activity relationships of celecoxib analogs are discussed, which may be beneficial in the design and development of novel analogs as potent antiproliferative agents in the future.

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Effects of celecoxib and L-NAME on apoptosis and cell cycle ofMCF-7 CD44+/CD24–/low subpopulation

Cited by 8 publications

References 21 publications

One Pot Doxorubicin Partitioning and Encapsulation on Silica Nanoparticle, Applying Aqueous Two Phase System for Preparation of pH-Responsive Nanocarriers

One Pot Doxorubicin Partitioning and Encapsulation on Silica Nanoparticle, Applying Aqueous Two Phase System for Preparation of pH-Responsive Nanocarriers

The effects of L-NAME on DU145 human prostate cancer cell line: A cytotoxicity-based study

Recent advances in the development of celecoxib analogs as anticancer agents: A review

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