Publications by authors named "Hemma H Schueffl"

Platinum chemotherapy is part of every second anticancer treatment regimen. However, its application is limited by severe side effects and drug resistance. The combination of platinum-based chemotherapeutics with EGFR inhibitors has shown remarkable synergism in clinical treatment.

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Article Synopsis
  • Small-molecule EGFR inhibitors have improved survival rates in EGFR-mutated lung cancer, but they often cause severe side effects and resistance.
  • A new prodrug, KP2334, selectively activates in tumor areas with low oxygen levels, releasing a novel EGFR inhibitor, KP2187, designed to work effectively in those regions.
  • Research shows that KP2187 has similar binding and inhibitory effects on EGFR as established drugs like erlotinib and gefitinib, and it also works well in combination with VEGFR inhibitors, suggesting it could reduce toxicity in combination therapies.
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A series of new Luotonin A derivatives with substituents at rings A and E was synthesized, together with some E-ring-unsubstituted derivatives. Subsequently, the compound library was examined in silico for their binding into a previously proposed site in the DNA/topoisomerase I binary complex. Whereas no convincing correlation between docking scores and biological data from in vitro assays could be found, one novel 4,9-diamino Luotonin A derivative had strong antiproliferative activity based on massive G2/M phase arrest.

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Following two orthogonal synthetic routes, a series of all four possible A-ring amino derivatives of the natural product Luotonin A (a known Topoisomerase I inhibitor) was synthesized. In both strategies, intramolecular cycloaddition reactions are the key step. The target compounds were obtained in good yields by mild catalytic transfer hydrogenation of the corresponding nitro precursors.

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Colorectal cancer (CRC) is one of the most commonly diagnosed cancers and a major cause of cancer mortality worldwide. At late stage of the disease CRC often shows (multiple) metastatic lesions in the peritoneal cavity which cannot be efficiently targeted by systemic chemotherapy. This is one major factor contributing to poor prognosis.

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