Mechanisms of porphyrinoid localization in tumors

Osterloh, Jens; Vicente, M. Graça H.

doi:10.1142/s1088424602000373

Cited by 101 publications

(78 citation statements)

References 186 publications

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“…Hydrophobic tetrapyrroles accumulate in cells through a variety of mechanisms, including passive diffusion, entry by flipping through the membrane, and association with serum proteins (11,26). Serum components, including albumin and LDL, have been shown to act as delivery vehicles for hydrophobic compounds through receptordependent and independent endocytosis, both leading to lysosomal accumulation (26)(27)(28).…”

Section: Resultsmentioning

confidence: 99%

“…Heteroatom-functionalized pzs have intense NIR absorption/emission (8) and recently have been considered as optical contrast agents for tumor detection and as a platform for cancer treatment using PDT (9,10). These pzs are synthetically flexible (8), making it possible to independently fine tune their NIR optical characteristics and amphiphilicity, a characteristic shown to dictate tumor retention of porphyrinoids (11,12).…”

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confidence: 99%

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Chiral porphyrazine near-IR optical imaging agent exhibiting preferential tumor accumulation

Trivedi

Harney

Olive

et al. 2009

Proc. Natl. Acad. Sci. U.S.A.

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A chiral porphyrazine (pz), H 2 [pz( trans - A 2 B 2 )] (247), has been prepared that exhibits preferential in vivo accumulation in the cells of tumors. Pz 247 exhibits near-infrared (NIR) emission with λ > 700 nm in the required wavelength range for maximum tissue penetration. When MDA-MB-231 breast tumor cells are treated with 247, the agent shows strong intracellular fluorescence with an emission maximum, 704 nm, which indicates that it localizes within a hydrophobic microenvironment. Pz 247 is shown to associate with the lipophilic core of LDL and undergo cellular entry primarily through receptor-mediated endocytosis accumulating in lysosomes. Preliminary in vivo studies show that 247 exhibits preferential accumulation and retention in the cells of MDA-MB-231 tumors subcutaneously implanted in mice, thereby enabling NIR optical imaging with excellent contrast between tumor and surrounding tissue. The intensity of fluorescence from 247 within the tumor increases over time up to 48 h after injection presumably due to the sequestration of circulating 247/LDL complex by the tumor tissue. As the need for cholesterol, and thus LDL, is elevated in highly proliferative tumor cells over nontumorigenic cells, 247 has potential application for all such tumors.

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Section: Resultsmentioning

confidence: 99%

mentioning

confidence: 99%

Chiral porphyrazine near-IR optical imaging agent exhibiting preferential tumor accumulation

Trivedi

Harney

Olive

et al. 2009

Proc. Natl. Acad. Sci. U.S.A.

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“…methyl-13(1)-desoxopyropheophorbide a (15) [55] were obtained according to literature procedures. Methyl-13(1)-hydroxy-13(1)desoxo-pheophorbide a (18), [57] chlorin e 6 13(1)-N-(2-hydroxyethyl)amide-15(3),17(3)-dimethyl ester (24), [58] chlorin e 6 13(1)-morpholinylamide-15(3),17(3)-dimethyl ester (25), [58] rodin g 7 13(1)-N,N-dimethylamide-15(3),17(3)-dimethyl ester (34), [59] chlorin e 6 13(1),17(3)-N,N'-(2-hydroxyethyl)diamide-15(3),17(3)-dimethyl ester (32), [60] and chlorin e 6 13(1),15(2),17(3)-N,N',N''-(2-hydroxyethyl)triamide (33) [60] were also obtained according to the known procedures.…”

Section: Methodsmentioning

confidence: 99%

“…[1][2][3][4][5][6] Thus, new PS searching among chlorophyll a derivatives is of a good chance and the investigation of their activity mechanisms and "structure-activity" regularities are of a great interest for new potential PS synthesis planning. [15,21,[28][29][30][31][32] Variation of chlorins chemical structure features such as charge, hydrophobicity and steric properties leads to the significant changing of the pigments ability to insert into the cell which can define their photodynamic effectivity. [33,34] The ability of pigments to interact with membrane structures is of a great significance for photosensitizing activity appearance in cell culture and in vivo.…”

Section: Introductionmentioning

confidence: 99%

Erythrocytes Membrane Photodestruction Sensitized Chlorophyll a Derivatives: Some Structure-Activity Regularities

Белых¹,

Шевченко²,

Tarabukina³

2014

MHC

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“…Дан-ные по химии и фотодинамической активности этих соединений, а также их многочисленных производных подробно рассмотрены в монографиях [1][2][3] и обзорных статьях. [4][5][6][7][8][9][10][11][12] На основе хлорина e 6 созданы препараты второго поколения Фотодитазин (Россия), Радахлорин (Россия), Фотолон (Республика Беларусь), моно-L-аспартилхлорин (Япония). В США в настоящее время проходит клинические испытания 3-(1´-гексилокси) этилпирофеофорбид a (HPPH).…”

Section: Introductionunclassified

Chlorin p6 Cycloimides: Syntheses, Properties and Possible Fields of Application

Lebedeva¹,

Ruziev²,

Миронов³

2012

MHC

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Mechanisms of porphyrinoid localization in tumors

Cited by 101 publications

References 186 publications

Chiral porphyrazine near-IR optical imaging agent exhibiting preferential tumor accumulation

Chiral porphyrazine near-IR optical imaging agent exhibiting preferential tumor accumulation

Erythrocytes Membrane Photodestruction Sensitized Chlorophyll a Derivatives: Some Structure-Activity Regularities

Chlorin p6 Cycloimides: Syntheses, Properties and Possible Fields of Application

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