Affiliation:
1. Molecular Sensors and Therapeutics (MST) Research Laboratory Department of Chemistry, School of Natural Sciences Shiv Nadar Institution of Eminence (SNIoE) Delhi NCR, NH 91, Tehsil Dadri Greater Noida Uttar Pradesh 201314 India
2. Protein Homeostasis Laboratory Department of Life Sciences School of Natural Sciences Shiv Nadar Institution of Eminence (SNIoE) Delhi NCR, NH 91, Tehsil Dadri Greater Noida Uttar Pradesh 201314 India
Abstract
AbstractMitochondria are the powerhouse of the cell and function at pH ∼8.0. Dysfunctions of mitochondria, includes mitochondrial damage, leading to pH alteration. Hence, researchers aim to develop efficient pH probes for tracking mitochondrial pH dynamics. Herein, we developed a PET‐based fluorescent probe for pH monitoring during mitochondrial dysfunctions. Three derivatives were synthesized with a variable spacer's length in pentacyclic pyridinium fluorophores (PM‐C2, PM‐C3, and PM‐C6). An efficient electron transfers from the receptor (tertiary amine) was observed in the case of PM‐C2 compared to the other two derivatives. This PET process was inhibited when tertiary amine was protonated in acidic pH. However, PM‐C3 showed minimal fluorescence intensity at similar conditions and almost negligible change in case of PM‐C6, suggesting poor PET process for both the derivatives. Furthermore, DFT/TD‐DFT quantum chemical calculation well supported this optical phenomena and PET process. Biocompatible, photostable, and mitochondria‐specific PM‐C2 could monitor pH dynamics during mitochondrial damage which were engulfed by lysosome, also known as mitophagy. This mitophagy process were induced by rapamycin and starvation, which can be monitored by turn‐on fluorescence enhancement. This process was further validated by tracking Parkin‐protein translocation from cytoplasm to damaged mitochondria using our developed probe.
Subject
General Chemistry,Biochemistry,Organic Chemistry
Cited by
4 articles.
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