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W4384207868 endingPage "108213" @default.
W4384207868 startingPage "108213" @default.
W4384207868 abstract "With almost 20 million new cases per year, cancer constitutes one of the most important challenges for public health systems. Unlike traditional chemotherapy, targeted anti-cancer strategies employ sophisticated therapeutics to precisely identify and attack cancer cells, limiting the impact of drugs on healthy cells and thereby minimizing the unwanted side effects of therapy. Protein drug conjugates (PDCs) are a rapidly growing group of targeted therapeutics, composed of a cancer-recognition factor covalently coupled to a cytotoxic drug. Several PDCs, mainly in the form of antibody-drug conjugates (ADCs) that employ monoclonal antibodies as cancer-recognition molecules, are used in the clinic and many PDCs are currently in clinical trials. Highly selective, strong and stable interaction of the PDC with the tumor marker, combined with efficient, rapid endocytosis of the receptor/PDC complex and its subsequent effective delivery to lysosomes, is critical for the efficacy of targeted cancer therapy with PDCs. However, the bivalent architecture of contemporary clinical PDCs is not optimal for tumor receptor recognition or PDCs internalization. In this review, we focus on multivalent PDCs, which represent a rapidly evolving and highly promising therapeutics that overcome most of the limitations of current bivalent PDCs, enhancing the precision and efficiency of drug delivery to cancer cells. We present an expanding set of protein scaffolds used to generate multivalent PDCs that, in addition to folding into well-defined multivalent molecular structures, enable site-specific conjugation of the cytotoxic drug to ensure PDC homogeneity. We provide an overview of the architectures of multivalent PDCs developed to date, emphasizing their efficacy in the targeted treatment of various cancers." @default.
W4384207868 created "2023-07-14" @default.
W4384207868 creator A5007090445 @default.
W4384207868 creator A5035981675 @default.
W4384207868 creator A5039639054 @default.
W4384207868 creator A5065096705 @default.
W4384207868 creator A5089534049 @default.
W4384207868 creator A5092464996 @default.
W4384207868 date "2023-10-01" @default.
W4384207868 modified "2023-10-14" @default.
W4384207868 title "Multivalent protein-drug conjugates – An emerging strategy for the upgraded precision and efficiency of drug delivery to cancer cells" @default.
W4384207868 cites W1528942864 @default.
W4384207868 cites W1568852071 @default.
W4384207868 cites W1758612015 @default.
W4384207868 cites W1789153697 @default.
W4384207868 cites W1801990738 @default.
W4384207868 cites W1899701704 @default.
W4384207868 cites W1954202239 @default.
W4384207868 cites W1964119722 @default.
W4384207868 cites W1964321121 @default.
W4384207868 cites W1965939484 @default.
W4384207868 cites W1966390946 @default.
W4384207868 cites W1968961303 @default.
W4384207868 cites W1969424287 @default.
W4384207868 cites W1971122340 @default.
W4384207868 cites W1973555453 @default.
W4384207868 cites W1975329765 @default.
W4384207868 cites W1975823945 @default.
W4384207868 cites W1976212255 @default.
W4384207868 cites W1976859231 @default.
W4384207868 cites W1981730803 @default.
W4384207868 cites W1982348345 @default.
W4384207868 cites W1982415753 @default.
W4384207868 cites W1982475432 @default.
W4384207868 cites W1982849241 @default.
W4384207868 cites W1986852088 @default.
W4384207868 cites W1988233765 @default.
W4384207868 cites W1996261598 @default.
W4384207868 cites W2003052374 @default.
W4384207868 cites W2004160151 @default.
W4384207868 cites W2004167192 @default.
W4384207868 cites W2005746614 @default.
W4384207868 cites W2010039421 @default.
W4384207868 cites W2011720055 @default.
W4384207868 cites W2012534247 @default.
W4384207868 cites W2016162029 @default.
W4384207868 cites W2016538025 @default.
W4384207868 cites W2016883388 @default.
W4384207868 cites W2018478612 @default.
W4384207868 cites W2019183242 @default.
W4384207868 cites W2019628879 @default.
W4384207868 cites W2019772485 @default.
W4384207868 cites W2022208182 @default.
W4384207868 cites W2025779348 @default.
W4384207868 cites W2035838265 @default.
W4384207868 cites W2037546764 @default.
W4384207868 cites W2041195053 @default.
W4384207868 cites W2041402908 @default.
W4384207868 cites W2041998309 @default.
W4384207868 cites W2042587442 @default.
W4384207868 cites W2043228552 @default.
W4384207868 cites W2051181331 @default.
W4384207868 cites W2055284666 @default.
W4384207868 cites W2056881172 @default.
W4384207868 cites W2059781302 @default.
W4384207868 cites W2060208116 @default.
W4384207868 cites W2065176466 @default.
W4384207868 cites W2067186466 @default.
W4384207868 cites W2068322045 @default.
W4384207868 cites W2069402857 @default.
W4384207868 cites W2071609648 @default.
W4384207868 cites W2078224854 @default.
W4384207868 cites W2082241802 @default.
W4384207868 cites W2084016093 @default.
W4384207868 cites W2084312697 @default.
W4384207868 cites W2085365699 @default.
W4384207868 cites W2088729407 @default.
W4384207868 cites W2090309798 @default.
W4384207868 cites W2092836319 @default.
W4384207868 cites W2097721584 @default.
W4384207868 cites W2098182642 @default.
W4384207868 cites W2108030846 @default.
W4384207868 cites W2114926334 @default.
W4384207868 cites W2114990525 @default.
W4384207868 cites W2117584556 @default.
W4384207868 cites W2121160715 @default.
W4384207868 cites W2122851718 @default.
W4384207868 cites W2126818937 @default.
W4384207868 cites W2133414187 @default.
W4384207868 cites W2134900594 @default.
W4384207868 cites W2141346487 @default.
W4384207868 cites W2149538041 @default.
W4384207868 cites W2151637473 @default.
W4384207868 cites W2161162374 @default.
W4384207868 cites W2163108389 @default.
W4384207868 cites W2163889515 @default.
W4384207868 cites W2166613409 @default.
W4384207868 cites W2172219847 @default.