Plantaricin BM-1 decreases viability of SW480 human colorectal cancer cells by inducing caspase-dependent apoptosis

Wang, He; Jin, Junhua; Pang, Xiao-Na; Zheng, Bin; Zhu, Jingxin; Hao, Yanling; Zhang, Hongxing; Xie, Yuanhong

doi:10.3389/fmicb.2022.1103600

Cited by 10 publications

(7 citation statements)

References 39 publications

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“…Direct treatment of colorectal cancer cells with butyrate has been shown to trigger apoptosis through activation of the JNK/AP-1 pathway [ 39 ]. In a separate study, butyrate treatment inhibited colony formation and cell migration while also inducing apoptosis through downregulation of homeostasis regulatory gene, thioredoxin-1 [ 40 ]. Though inducing cell death in cancer cells, butyrate enhances the tumoricidal properties of T cells.…”

Section: Emerging Anticancer Agents From Microbial Metabolitesmentioning

confidence: 99%

Redefining bioactive small molecules from microbial metabolites as revolutionary anticancer agents

Giurini,

Godla,

Gupta

2024

Cancer Gene Ther

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Cancer treatment remains a significant challenge due to issues such as acquired resistance to conventional therapies and the occurrence of adverse treatment-related toxicities. In recent years, researchers have turned their attention to the microbial world in search of novel and effective drugs to combat this devastating disease. Microbial derived secondary metabolites have proven to be a valuable source of biologically active compounds, which exhibit diverse functions and have demonstrated potential as treatments for various human diseases. The exploration of these compounds has provided valuable insights into their mechanisms of action against cancer cells. In-depth studies have been conducted on clinically established microbial metabolites, unraveling their anticancer properties, and shedding light on their therapeutic potential. This review aims to comprehensively examine the anticancer mechanisms of these established microbial metabolites. Additionally, it highlights the emerging therapies derived from these metabolites, offering a glimpse into the immense potential they hold for anticancer drug discovery. Furthermore, this review delves into approved treatments and major drug candidates currently undergoing clinical trials, focusing on specific molecular targets. It also addresses the challenges and issues encountered in the field of anticancer drug research and development. It also presents a comprehensive exposition of the contemporary panorama concerning microbial metabolites serving as a reservoir for anticancer agents, thereby illuminating their auspicious prospects and the prospect of forthcoming strides in the domain of cancer therapeutics.

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Section: Emerging Anticancer Agents From Microbial Metabolitesmentioning

confidence: 99%

Redefining bioactive small molecules from microbial metabolites as revolutionary anticancer agents

Giurini,

Godla,

Gupta

2024

Cancer Gene Ther

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“…Plantarisin BM-1, a bacteriocin produced by Lactobacillus plantarum , significantly reduces the viability of SW480, Caco-2, and HCT-116 CRC cells, with a more pronounced impact on SW480 [ 147 ]. In a study that screened 16,000 bacterial clones from human fecal samples, salivaricin A5 and salivaricin B 243, the bacteriocins of Streptococcus salivarius , were shown to have selective antimicrobial activity against pro-tumorigenic Fusobacterium nucleatum strains and are a biotherapeutic that can target pathogens causing CRC [ 148 ].…”

Section: Postbiotics and Crcmentioning

confidence: 99%

The Crucial Roles of Diet, Microbiota, and Postbiotics in Colorectal Cancer

Kuru-Yaşar,

Üstün-Aytekin

2024

Curr Nutr Rep

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Purpose of Review Colorectal cancer is the second deadliest cancer in the world, and its prevalence has been increasing alarmingly in recent years. After researchers discovered the existence of dysbiosis in colorectal cancer, they considered the use of probiotics in the treatment of colorectal cancer. However, for various reasons, including the low safety profile of probiotics in susceptible and immunocompromised patient5s, and the risk of developing antibiotic resistance, researchers have shifted their focus to non-living cells, their components, and metabolites. This review aims to comprehensively evaluate the literature on the effects of diet, microbiota, and postbiotics on colorectal cancer and the future of postbiotics. Recent Findings The link between diet, gut microbiota, and colorectal cancer has been established primarily as a relationship rather than a cause-effect relationship. The gut microbiota can convert gastrointestinal tract and dietary factors into either onco-metabolites or tumor suppressor metabolites. There is serious dysbiosis in the microbiota in colorectal cancer. Postbiotics appear to be promising agents in the prevention and treatment of colorectal cancer. Summary It has been shown that various postbiotics can selectively induce apoptosis in CRC, inhibit cell proliferation, growth, invasion, and migration, modulate the immune system, suppress carcinogenic signaling pathways, maintain intestinal epithelial integrity, and have a synergistic effect with chemotherapy drugs. However, it is also reported that some postbiotics are ineffective and may be risky in terms of safety profile in some patients. Many issues need to be researched about postbiotics. Large-scale, randomized, double-blind clinical studies are needed.

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“…Interfered with the mechanisms of drug resistance [116]. Cancer cell death via a caspase-dependent pathway [117].…”

Section: Huh-7 and Snu182 Hepatocarcinomamentioning

confidence: 99%

Friend or Foe: Exploring the Relationship between the Gut Microbiota and the Pathogenesis and Treatment of Digestive Cancers

Profir,

Roşu,

Creţoiu

et al. 2024

Microorganisms

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Digestive cancers are among the leading causes of cancer death in the world. However, the mechanisms of cancer development and progression are not fully understood. Accumulating evidence in recent years pointing to the bidirectional interactions between gut dysbiosis and the development of a specific type of gastrointestinal cancer is shedding light on the importance of this “unseen organ”—the microbiota. This review focuses on the local role of the gut microbiota imbalance in different digestive tract organs and annexes related to the carcinogenic mechanisms. Microbiota modulation, either by probiotic administration or by dietary changes, plays an important role in the future therapies of various digestive cancers.

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Plantaricin BM-1 decreases viability of SW480 human colorectal cancer cells by inducing caspase-dependent apoptosis

Cited by 10 publications

References 39 publications

Redefining bioactive small molecules from microbial metabolites as revolutionary anticancer agents

Redefining bioactive small molecules from microbial metabolites as revolutionary anticancer agents

The Crucial Roles of Diet, Microbiota, and Postbiotics in Colorectal Cancer

Friend or Foe: Exploring the Relationship between the Gut Microbiota and the Pathogenesis and Treatment of Digestive Cancers

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