Aileen Shieh scite author profile

20-(S)-Camptothecin (CPT)-conjugated dipeptides are reported that preassemble into nanotubes with diameters ranging from 80-120 nm. These nanoassemblies maintain a high (∼47 %) drug loading and exhibit greater drug stability (i.e., resistance to lactone hydrolysis), and consequently greater efficacy against several human cancer cells (HT-29, A549, H460, and H23) in vitro compared with the clinically used prodrug irinotecan. A key and defining feature of this system is the use of the CPT-conjugated dipeptide as both the drug and precursor to the nanostructured carrier, which simplifies the overall fabrication process.

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Self-assembly of a 5-fluorouracil-dipeptide hydrogel

Sun

Kaplan

Shieh

et al. 2016

Chem. Commun.

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The self-assembly of 5-fluorouracil dilysine conjugates into self-supporting hydrogels, comprised of entangled nanofibers or rigid nanotubes with diameters of 10 and 16 nm, respectively, is reported. The rate of release of 5-Fu from the conjugates was highly dependent on concentration in solution, whereas, release from the fully formed hydrogels was significantly slower. The 5-Fu conjugate also exhibited promising in vitro cytotoxicity against human tumor cell lines A549, H460 and H23.

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Controlling the length of self-assembled nanotubes by sonication followed by polymer wrapping

Daniels

Shieh

et al. 2017

Chem. Commun.

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The self-assembly of a camptothecin-lysine nanotube

Sun

Shieh

Kim

et al. 2016

Bioorganic & Medicinal Chemistry Letters

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Aileen Shieh

The Self‐Assembly of Anticancer Camptothecin–Dipeptide Nanotubes: A Minimalistic and High Drug Loading Approach to Increased Efficacy

Self-assembly of a 5-fluorouracil-dipeptide hydrogel

Controlling the length of self-assembled nanotubes by sonication followed by polymer wrapping

The self-assembly of a camptothecin-lysine nanotube

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