Photoredox catalysis may be a general mechanism in photodynamic therapy

Li, Mingle; Xu, Yunjie; Zhang, Pu; Xiong, Tao; Huang, Haiqiao; Long, Saran; Son, Subin; Yu, Le; Singh, Nem; Tong, Yunkang; Sessler, Jonathan L.; Peng, Xiaojun; Kim, Jong Seung

doi:10.1073/pnas.2210504119

Cited by 31 publications

(29 citation statements)

References 34 publications

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“…Importantly, in living breast CSC-like SKBR3 cells, such a rapid release was also seen, and the reaction occurred in the mitochondria, as evidenced by colocalized fluorescence imaging between released resorufin and MitoTracker DiOC6 (Figure S15). In the presence of NAC ( N -acetyl- l -cysteine, a ROS scavenger), however, the fluorescence “On” signal in the mitochondria was markedly inhibited (Figure S15). These findings are consistent with the design expectation that Bo-Mt-Ge can localize to the mitochondria and be conditionally activated by peroxide in living cells.…”

Section: Resultsmentioning

confidence: 99%

Cutting Off H⁺ Leaks on the Inner Mitochondrial Membrane: A Proton Modulation Approach to Selectively Eradicate Cancer Stem Cells

et al. 2023

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Cancer stem cells (CSCs) are associated with the invasion and metastatic relapse of various cancers. However, current cancer therapies are limited to targeting the bulk of primary tumor cells while remaining the CSCs untouched. Here, we report a new proton (H+) modulation approach to selectively eradicate CSCs via cutting off the H+ leaks on the inner mitochondrial membrane (IMM). Based on the fruit extract of Gardenia jasminoides, a multimodal molecule channel blocker with high biosafety, namely, Bo-Mt-Ge, is developed. Importantly, in this study, we successfully identify that mitochondrial uncoupling protein UCP2 is closely correlated with the stemness of CSCs, which may offer a new perspective for selective CSC drug discovery. Mechanistic studies show that Bo-Mt-Ge can specifically inhibit the UCP2 activities, decrease the H+ influx in the matrix, regulate the electrochemical gradient, and deplete the endogenous GSH, which synergistically constitute a unique MoA to active apoptotic CSC death. Intriguingly, Bo-Mt-Ge also counteracts the therapeutic resistance via a two-pronged tactic: drug efflux pump P-glycoprotein downregulation and antiapoptotic factor (e.g., Bcl-2) inhibition. With these merits, Bo-Mt-Ge proved to be one of the safest and most efficacious anti-CSC agents, with ca. 100-fold more potent than genipin alone in vitro and in vivo. This study offers new insights and promising solutions for future CSC therapies in the clinic.

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Section: Resultsmentioning

confidence: 99%

Cutting Off H⁺ Leaks on the Inner Mitochondrial Membrane: A Proton Modulation Approach to Selectively Eradicate Cancer Stem Cells

et al. 2023

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“…(2) Will photoredox biological catalysis be nextgeneration phototherapy? Artificial photoredox catalysis-based cancer therapy is a rather new addition to the ever-expanding PDT community (as the results show in our JACS 4 and PNAS papers 5 ). This hence provides a large scope for further contributions in terms of both developing biologically benign photocatalysts and exploring new photoredox reactions in living systems.…”

Section: Discussionmentioning

confidence: 99%

“…Motivated by these findings, we were curious about how general this MoA (i.e., photoredox catalysis) would be in PDT and surprisingly found that common PSs, such as transition metal complex, BODIPY, Rose Bengal, porphyrin, and phthalocyanine, are all capable of triggering a photoredox NADH catalysis, which means that "photoredox catalysis in cells" might be a general mechanism behind PDT (Figure 11). 5 We believe that exploring the power of artificial photoredox chemistry in the biomedical area would open unforeseen opportunities for metabolic or genetic interventions and unveil new photochemical techniques for clinical disease diagnosis and therapy.…”

Section: O 2 -Independent Photoredox Catalysismentioning

confidence: 99%

“…Photodynamic therapy (PDT), a photon-triggered therapeutic strategy that involves the synergistic utilization of light, photosensitizer (PS), and molecular oxygen (O 2 ) to produce cytotoxic reactive oxygen species (ROS) and eradicate localized tumor cells, has garnered ever-increasing attention in clinical cancer therapy. − It has unique merits such as minimal invasiveness, remote control, and fast and cost-efficient operation. In some situations, PDT has even been demonstrated to be effective where treatments like surgery, chemical therapy, and radiation therapy have failed.…”

Section: Introductionmentioning

confidence: 99%

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From Low to No O₂-Dependent Hypoxia Photodynamic Therapy (hPDT): A New Perspective

Peng

et al. 2022

Acc. Chem. Res.

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Conspectus The advent of photochemical techniques has revolutionized the landscape of biology and medical sciences. Especially appealing in this context is photodynamic therapy (PDT), which is a photon-initiated treatment modality that uses cytotoxic reactive oxygen species (ROS) to kill malignant cells. In the past decade, PDT has risen to the forefront of cancer therapy. Its optical control enables noninvasive and spatiotemporal manipulation of the treatment process, and its photoactive nature allows unique patterns to avoid drug resistance to conventional chemotherapeutics. However, despite the impressive advances in this field, achieving widespread clinical adoption of PDT remains difficult. A major concern is that in the hostile tumor microenvironment, tumor cells are hypoxic, which hinders ROS generation during PDT action. To overcome this “Achilles’ heel”, current strategies focus primarily on the improvement of the intratumoral O2 perfusion, while clinical trials suggest that O2 enrichment may promote cancer cell proliferation and metastasis, thereby making FDA approval and clinical transformation of these paradigms challenging. In an effort to improve hypoxia photodynamic therapy (hPDT) in the clinic, we have explored “low to no O2-dependent” photochemical approaches over the years to combat hypoxia-induced resistance. In this Account, we present our contributions to this theme during the past 5 years, beginning with low O2-dependent approaches (e.g., type I superoxide radical (O2 •–) generator, photodynamic O2-economizer, mitochondrial respiration inhibition, cellular self-protective pathway modulation, etc.) and progressing to O2-independent strategies (e.g., autoadaptive PDT/PTT complementary therapy, O2-independent artificial photoredox catalysis in cells). These studies have attracted tremendous attention. Particularly in the pioneering work of 2018, we presented the first demonstration that the O2 •–-mediated partial O2-recyclability mechanism can overcome PDT resistance (J. Am. Chem. Soc.20181401485114859). This launched an era of renewed interest in type I PDT, resulting in a plethora of new O2 •– photogenerators developed by many groups around the world. Moreover, with the discovery of O2-independent photoredox reactions in living cells, artificial photoredox catalysis has emerged as a new field connecting photochemistry and biomedicine, stimulating the development of next-generation phototherapeutic tools (J. Am. Chem. Soc.2022144163173). Our recent work also disclosed that “photoredox catalysis in cells” might be a general mechanism of action of PDT (e2210504119Proc. Natl. Acad. Sci. U.S.A.2022119). These emergent concepts, molecular designs, photochemical mechanisms, and applications in cancer diagnosis and therapeutics, as well as pros and cons, are discussed in depth in this Account. It is expected that our contributions to date will be of general use to researchers and inspire future efforts to identify more promising hPDT approaches that better meet the clinical needs of cancer therapy.

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“…Photodynamic therapy (PDT) has attracted great attention in curing cancers due to its minimal invasiveness and side effects, spatiotemporal selectivity, and high therapeutic efficacy compared to conventional cancer treatments. − In PDT, the photoexcited photosensitizers (PSs) convert triplet oxygen and other molecules into cytotoxic reactive oxygen species (ROS) via electron transfer (type-I) or energy transfer (type-II), which subsequently induce apoptosis or necrosis of tumor cells. − However, the high hydrophobicity-caused aggregation of PSs under physiological conditions usually results in significant self-quenching of excitons, thereby decreasing their ROS generation efficacy severely. ,, Additionally, the hypoxic microenvironment of solid tumors further hinders most type-II PSs from achieving satisfactory in vivo PDT performance. ,,− …”

Section: Introductionmentioning

confidence: 99%

Boosting Type-I and Type-II ROS Production of Water-Soluble Porphyrin for Efficient Hypoxic Tumor Therapy

et al. 2022

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As the most successful clinically approved photosensitizers, porphyrins have been extensively employed in the photodynamic therapy (PDT) of cancers. However, their poor water solubility, aggregation-induced self-quenching on ROS generation, and a low tolerance for a hypoxic condition usually result in unsatisfied therapeutic outcomes. Therefore, great efforts have been dedicated to improving the PDT efficacy of porphyrin-type photosensitizers in treating hypoxic tumors, including combination with additional active components or therapies, which can significantly complicate the therapeutic process. Herein, we report a novel water-soluble porphyrin with O-linked cationic side chains, which exhibits good water solubility, high photostability, and significantly enhanced ROS generation efficacy in both type-I and type-II photodynamic pathways. We have also found that the end charges of side chains can dramatically affect the ROS generation of the porphyrin. The cationic porphyrin exhibited high in vitro PDT efficacy with low IC50 values both in normoxia and hypoxia. Hence, during in vivo PDT study, the cationic porphyrin displayed highly effective tumor ablation capability. This study demonstrates the power of side-chain chemistry in tuning the photodynamic property of porphyrin, which offers a new effective strategy to enhance the anticancer performance of photosensitizers for fulfilling the increasing demands for cancer therapy in clinics.

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Photoredox catalysis may be a general mechanism in photodynamic therapy

Cited by 31 publications

References 34 publications

Cutting Off H⁺ Leaks on the Inner Mitochondrial Membrane: A Proton Modulation Approach to Selectively Eradicate Cancer Stem Cells

Cutting Off H⁺ Leaks on the Inner Mitochondrial Membrane: A Proton Modulation Approach to Selectively Eradicate Cancer Stem Cells

From Low to No O₂-Dependent Hypoxia Photodynamic Therapy (hPDT): A New Perspective

Boosting Type-I and Type-II ROS Production of Water-Soluble Porphyrin for Efficient Hypoxic Tumor Therapy

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Photoredox catalysis may be a general mechanism in photodynamic therapy

Cited by 31 publications

References 34 publications

Cutting Off H+ Leaks on the Inner Mitochondrial Membrane: A Proton Modulation Approach to Selectively Eradicate Cancer Stem Cells

Cutting Off H+ Leaks on the Inner Mitochondrial Membrane: A Proton Modulation Approach to Selectively Eradicate Cancer Stem Cells

From Low to No O2-Dependent Hypoxia Photodynamic Therapy (hPDT): A New Perspective

Boosting Type-I and Type-II ROS Production of Water-Soluble Porphyrin for Efficient Hypoxic Tumor Therapy

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Resources

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Cutting Off H⁺ Leaks on the Inner Mitochondrial Membrane: A Proton Modulation Approach to Selectively Eradicate Cancer Stem Cells

Cutting Off H⁺ Leaks on the Inner Mitochondrial Membrane: A Proton Modulation Approach to Selectively Eradicate Cancer Stem Cells

From Low to No O₂-Dependent Hypoxia Photodynamic Therapy (hPDT): A New Perspective