2016
DOI: 10.1021/acs.bioconjchem.6b00291
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Natural Product Splicing Inhibitors: A New Class of Antibody–Drug Conjugate (ADC) Payloads

Abstract: There is a considerable ongoing work to identify new cytotoxic payloads that are appropriate for antibody-based delivery, acting via mechanisms beyond DNA damage and microtubule disruption, highlighting their importance to the field of cancer therapeutics. New modes of action will allow a more diverse set of tumor types to be targeted and will allow for possible mechanisms to evade the drug resistance that will invariably develop to existing payloads. Spliceosome inhibitors are known to be potent antiprolifera… Show more

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Cited by 58 publications
(53 citation statements)
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“…Eight randomized animals were dosed intravenously at 3mg/kg on days 0, 4, 8 and 12 (q4d x 4) when the tumor size reached approximately 350 mm 3 . In contrast to the excellent potency previously reported for DAR4 lysine thialanstatin conjugates [19], only a modest reduction in tumor growth rate was observed in comparison to a vehicle control (Fig 1C). …”
Section: Resultscontrasting
confidence: 91%
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“…Eight randomized animals were dosed intravenously at 3mg/kg on days 0, 4, 8 and 12 (q4d x 4) when the tumor size reached approximately 350 mm 3 . In contrast to the excellent potency previously reported for DAR4 lysine thialanstatin conjugates [19], only a modest reduction in tumor growth rate was observed in comparison to a vehicle control (Fig 1C). …”
Section: Resultscontrasting
confidence: 91%
“…The cytotoxicity and selectivity of these ADCs ( ADC1-3 ) were assessed against several cancer cell lines with varying levels of Her2 expression (Fig 1B). Similar to our earlier published results [19], all the hinge cysteine conjugates of thailanstatin displayed potent activity (IC 50 ~1 nM) against the high Her2 (>600,000 receptors/cell) expressing N87 gastric cancer cell line but were not potent against moderate antigen expressing MDA-MB-361-DYT2 (361) breast cancer cell line (~150,000 receptors/cell). As expected, all ADCs were inactive against a non-antigen expressing cell lines, MDA-MB-468 (468).…”
Section: Resultssupporting
confidence: 89%
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“…Recent publications on new payload and linkers, although still sparse, along with understanding of the mechanism of action of ADCs, are encouraging signs that chemistry efforts to optimize ADCs are being prioritized and that some progress is now being made. 11,12 ■ AUTHOR INFORMATION Corresponding Author *E-mail: ravi.chari@immunogen.com. …”
Section: Acs Medicinal Chemistry Lettersmentioning
confidence: 99%