Evidence for distinct mechanisms of uptake and antitumor activity of secretory phospholipase A2 responsive liposome in prostate cancer

Mock, Jason N.; Costyn, Leah J.; Wilding, S. L.; Arnold, Robert D.; Cummings, Brian S.

doi:10.1039/c2ib20108a

Cited by 47 publications

(48 citation statements)

References 29 publications

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“…Recent studies, including those from our own laboratory, have engineered liposomes to target pathologies that overexpress sPLA 2 and enhance the release of drugs at diseased tissue [87-89]. sPLA 2 -targeted nanoparticles are composed of phospholipids that are preferentially cleaved by sPLA 2 , such as those with negatively charged and altered levels of phospholipids containing other zwitterionic head groups and shorter fatty acyl chains [89-91].…”

Section: Therapies Targeting Spla2mentioning

confidence: 99%

“…sPLA 2 -targeted nanoparticles are composed of phospholipids that are preferentially cleaved by sPLA 2 , such as those with negatively charged and altered levels of phospholipids containing other zwitterionic head groups and shorter fatty acyl chains [89-91]. This preference is likely a result of the many positively charge amino acids present in sPLA 2 ’s protein sequence (Figure 2B-D), especially at the ICS where these residues are believed to increase the interaction with the negatively charged phospholipid head group.…”

Section: Therapies Targeting Spla2mentioning

confidence: 99%

“…There have been many proposed modifications of the phospholipid component of liposomes to improve drug release at sPLA 2 -targeted sites [87, 89]. One such modification was the incorporation of low (> 10%) amount of zwitterionic phosphatidylethanolamine (PE) into sterically stable liposomes (SSL).…”

Section: Therapies Targeting Spla2mentioning

confidence: 99%

“…One such modification was the incorporation of low (> 10%) amount of zwitterionic phosphatidylethanolamine (PE) into sterically stable liposomes (SSL). These modified liposomes, termed sPLA 2 responsive liposomes (SPRL), showed enhanced drug release in the presence of Group IIA and III sPLA 2 , and were more effective than SSL (which are similar to clinically used formulations) in limiting hormone refractory prostate cancer tumor growth in mouse models [89]. One interesting finding with SPRL is that their activity or effectiveness was not altered by LY3711727.…”

Section: Therapies Targeting Spla2mentioning

confidence: 99%

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Secretory phospholipase A2 enzymes as pharmacological targets for treatment of disease

Quach

Arnold

Cummings

2014

Biochemical Pharmacology

155

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Phospholipase A2 (PLA2) cleave phospholipids preferentially at the sn-2 position, liberating free fatty acids and lysophospholipids. They are classified into six main groups based on size, location, function, substrate specificity and calcium requirement. These classes include secretory PLA2 (sPLA2), cytosolic (cPLA2), Ca2+-independent (iPLA2), platelet activating factor acetylhydrolases (PAF-AH), lysosomal PLA2 (LyPLA2) and adipose specific PLA2 (AdPLA2). It is hypothesized that PLA2 can serve as pharmacological targets for the therapeutic treatment of several diseases, including cardiovascular diseases, atherosclerosis, immune disorders and cancer. Special emphasis has been placed on inhibitors of sPLA2 isoforms as pharmacological moieties, mostly due to the fact that these enzymes are activated during inflammatory events and because their expression is increased in several diseases. This review focuses on understanding how sPLA2 isoform expression is altered during disease progression and the possible therapeutic interventions to specifically target sPLA2 isoforms, including new approaches using nano-particulate-based strategies.

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Section: Therapies Targeting Spla2mentioning

confidence: 99%

Section: Therapies Targeting Spla2mentioning

confidence: 99%

Section: Therapies Targeting Spla2mentioning

confidence: 99%

Section: Therapies Targeting Spla2mentioning

confidence: 99%

See 2 more Smart Citations

Secretory phospholipase A2 enzymes as pharmacological targets for treatment of disease

Quach

Arnold

Cummings

2014

Biochemical Pharmacology

155

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“…[199][200][201] Liposomes that are responsible for sPLA2 (SPRL) were engineered to facilitate liposomal degradation and drug release in tumor tissues. [202][203][204] In a study comparing the uptakes and cytotoxicities of the SPRL encapsulated with DOX and sterically stabilized liposomes encapsulated with DOX, Moch et al suggested that the efficacy of the sPLA2 liposomes are mediated by cell-dependent mechanisms. 203 Recently, Hofmann et al provided evidence supporting the existence of drug delivery into cells without cellular uptake of the nanoparticles through a new "kiss-andrun" mechanism between (polymeric) nanoparticles and the cell membrane.…”

mentioning

confidence: 99%

Overcoming tumor cell chemoresistance using nanoparticles: lysosomes are beneficial for (stearoyl) gemcitabine-incorporated solid lipid nanoparticles

Chen¹,

Zheng²,

Shi³

et al. 2018

IJN

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Despite recent advances in targeted therapies and immunotherapies, chemotherapy using cytotoxic agents remains an indispensable modality in cancer treatment. Recently, there has been a growing emphasis in using nanomedicine in cancer chemotherapy, and several nanomedicines have already been used clinically to treat cancers. There is evidence that formulating small molecular cancer chemotherapeutic agents into nanomedicines significantly modifies their pharmacokinetics and often improves their efficacy. Importantly, cancer cells often develop resistance to chemotherapy, and formulating anticancer drugs into nanomedicines also helps overcome chemoresistance. In this review, we briefly describe the different classes of cancer chemotherapeutic agents, their mechanisms of action and resistance, and evidence of overcoming the resistance using nanomedicines. We then emphasize on gemcitabine and our experience in discovering the unique (stearoyl) gemcitabine solid lipid nanoparticles that are effective against tumor cells resistant to gemcitabine and elucidate the underlying mechanisms. It seems that lysosomes, which are an obstacle in the delivery of many drugs, are actually beneficial for our (stearoyl) gemcitabine solid lipid nanoparticles to overcome tumor cell resistance to gemcitabine.

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Interfacing Materials Science and Biology for Drug Carrier Design

et al. 2015

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Over the last ten years, there has been considerable research interest in the development of polymeric carriers for biomedicine. Such delivery systems have the potential to significantly reduce side effects and increase the bioavailability of poorly soluble therapeutics. The design of carriers has relied on harnessing specific variations in biological conditions, such as pH or redox potential, and more recently, by incorporating specific peptide cleavage sites for enzymatic hydrolysis. Although much progress has been made in this field, the specificity of polymeric carriers is still limited when compared with their biological counterparts. To synthesize the next generation of carriers, it is important to consider the biological rationale for materials design. This requires a detailed understanding of the cellular microenvironments and how these can be harnessed for specific applications. In this review, several important physiological cues in the cellular microenvironments are outlined, with a focus on changes in pH, redox potential, and the types of enzymes present in specific regions. Furthermore, recent studies that use such biologically inspired triggers to design polymeric carriers are highlighted, focusing on applications in the field of therapeutic delivery.

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Evidence for distinct mechanisms of uptake and antitumor activity of secretory phospholipase A2 responsive liposome in prostate cancer

Cited by 47 publications

References 29 publications

Secretory phospholipase A2 enzymes as pharmacological targets for treatment of disease

Secretory phospholipase A2 enzymes as pharmacological targets for treatment of disease

Overcoming tumor cell chemoresistance using nanoparticles: lysosomes are beneficial for (stearoyl) gemcitabine-incorporated solid lipid nanoparticles

Interfacing Materials Science and Biology for Drug Carrier Design

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