Translocation of Platinum Anticancer Drugs by Human Copper ATPases ATP7A and ATP7B

Tadini‐Buoninsegni, Francesco; Bartolommei, Gianluca; Moncelli, Maria Rosa; Inesi, Giuseppe; Galliani, Angela; Sinisi, Marilù; Losacco, Maurizio; Natile, Giovanni; Arnesano, Fabio

doi:10.1002/ange.201307718

Cited by 19 publications

(29 citation statements)

References 16 publications

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“…ATP7A mediates the transport of platinum drugs across the cellular membranes, and is considered to sequester platinum agents in intracellular compartments and to prevent their reaction with nuclear DNA [24,25]. A correlation between the expression of ATP7A and the degree of acquired resistance to platinum drug in cultured cells and tumor samples suggests that the copper transporters are important constituents of the program that regulates sensitivity to platinum drugs [26,27]. ATP7A C2299G, mutated in high frequency of 23.2 % in Chinese population, can change the gene functions.…”

Section: Discussionmentioning

confidence: 99%

Clinical outcome of cisplatin-based chemotherapy is associated with the polymorphisms of GSTP1 and XRCC1 in advanced non-small cell lung cancer patients

et al. 2015

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Section: Discussionmentioning

confidence: 99%

Clinical outcome of cisplatin-based chemotherapy is associated with the polymorphisms of GSTP1 and XRCC1 in advanced non-small cell lung cancer patients

et al. 2015

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“…All MBDs of these ATPases share a high sequence homology and exhibit similar protein folding with a conserved Cu I ‐binding motif CXXC . In addition, all of the MBDs show similar binding affinity to cuprous ion .…”

Section: Figurementioning

confidence: 96%

“…It has been reported that pre‐loading with Cu can enhance the platination of copper chaperones Atox1 and Cox17, in spite of the fact that Pt II and Cu I bind to the same coordination site . In order to investigate the effect of Cu I on the platination of these ATPases, the reaction with cisplatin was conducted on Cu‐loaded proteins.…”

Section: Figurementioning

confidence: 99%

“…The reaction of apo‐MNK6 with cisplatin generates two chromatographic peaks falling at 11 and 13 mL retention volumes; in contrast only one peak at 9 mL retention volume is generated in the case of Cu‐MNK6 (Figure C and D). The two peaks observed in the case of apo‐MNK6 could be due to formation of a monofunctional and a bifunctional platinum adduct, as observed in a previous work on MNK1 . Thus, these results also fully confirm the fluorescence data, indicating that the reaction rate is dependent upon the nature of the MBD and of its loading with Cu.…”

Section: Figurementioning

confidence: 99%

“…As mentioned in the introduction, the expression level of Cu‐ATPases positively correlates with cisplatin resistance of cancer cells . It was also demonstrated that ATP7A/B can translocate cisplatin or oxaliplatin in an ATP‐dependent way . The translocation in the case of Pt II occurs with a rate comparable to that of Cu I and with equal amount of positive charge displaced upon ATP utilization within a single catalytic cycle.…”

Section: Figurementioning

confidence: 99%

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Differential Reactivity of Metal Binding Domains of Copper ATPases towards Cisplatin and Colocalization of Copper and Platinum

Fang

Tian

Yuan

et al. 2018

Chemistry A European J

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The Menkes (MNK) and Wilson (WLN) disease proteins are two P-type ATPases responsible for active Cu efflux. These ATPases are also associated with resistance to cisplatin. In this work, different metal-binding domains (MBDs) of ATPases (9 out of 12 domains) were compared based on their reactivity towards cisplatin. The reaction rates of the MBDs can be largely different; the reaction of MNK6 is about six times faster than that of WLN2. Copper coordination favors the platination of the MBDs to different extents. The rate of platination was generally greater for holo-MBDs than for apo-MBDS (particularly in the case of WLN4 and WLN2); however, it was negligibly affected in the case of MNK6. Interestingly, the platinum binding weakens the Cu coordination, but does not expel the copper ion from MBDs. The latter results nicely explain the inhibitory effect of Cu upon the cisplatin translocation promoted by Cu-ATPases and can help in understanding how copper levels can modulate the sensitivity of cancer cells to platinum chemotherapy.

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Computational Library Design for Increasing Haloalkane Dehalogenase Stability

et al. 2014

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We explored the use of a computational design framework for the stabilization of the haloalkane dehalogenase LinB. Energy calculations, disulfide bond design, molecular dynamics simulations, and rational inspection of mutant structures predicted many stabilizing mutations. Screening of these in small mutant libraries led to the discovery of seventeen point mutations and one disulfide bond that enhanced thermostability. Mutations located in or contacting flexible regions of the protein had a larger stabilizing effect than mutations outside such regions. The combined introduction of twelve stabilizing mutations resulted in a LinB mutant with a 23 °C increase in apparent melting temperature (Tm,app , 72.5 °C) and an over 200-fold longer half-life at 60 °C. The most stable LinB variants also displayed increased compatibility with co-solvents, thus allowing substrate conversion and kinetic resolution at much higher concentrations than with the wild-type enzyme.

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Translocation of Platinum Anticancer Drugs by Human Copper ATPases ATP7A and ATP7B

Cited by 19 publications

References 16 publications

Clinical outcome of cisplatin-based chemotherapy is associated with the polymorphisms of GSTP1 and XRCC1 in advanced non-small cell lung cancer patients

Clinical outcome of cisplatin-based chemotherapy is associated with the polymorphisms of GSTP1 and XRCC1 in advanced non-small cell lung cancer patients

Differential Reactivity of Metal Binding Domains of Copper ATPases towards Cisplatin and Colocalization of Copper and Platinum

Computational Library Design for Increasing Haloalkane Dehalogenase Stability

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