Publication | Open Access
Alkyne-tagged SERS nanoprobe for understanding Cu+ and Cu2+ conversion in cuproptosis processes
38
Citations
43
References
2024
Year
Simultaneously quantifying mitochondrial Cu<sup>+</sup> and Cu<sup>2+</sup> levels is crucial for evaluating the molecular mechanisms of copper accumulation-involved pathological processes. Here, a series of molecules containing various diacetylene derivatives as Raman reporters are designed and synthesized, and the alkyne-tagged SERS probe is created for determination Cu<sup>+</sup> and Cu<sup>2+</sup> with high selectivity and sensitivity. The developed SERS probe generates well-separated distinguishable Raman fingerprint peaks with built-in corrections in the cellular silent region, resulting in accurate quantification of Cu<sup>+</sup> and Cu<sup>2+</sup>. The present probe demonstrates high tempo-spatial resolution for real-time imaging and simultaneously quantifying mitochondrial Cu<sup>+</sup> and Cu<sup>2+</sup> with long-term stability benefiting from the probe assembly with designed Au-C≡C groups. Using this powerful tool, it is found that mitochondrial Cu<sup>+</sup> and Cu<sup>2+</sup> increase during ischemia are associated with breakdown of proteins containing copper as well as conversion of Cu<sup>+</sup> and Cu<sup>2+</sup>. Meanwhile, we observe that parts of Cu<sup>+</sup> and Cu<sup>2+</sup> are transported out of neurons by ATPase. More importantly, cuproptosis in neurons is found including the oxidative stress process caused by the conversion of Cu<sup>+</sup> to Cu<sup>2+</sup>, which dominates at the early stage (<9 h), and subsequent proteotoxic stress. Both oxidative and proteotoxic stresses contribute to neuronal death.
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