A novel cyclic mobile transporter can induce apoptosis by facilitating chloride anion transport into cells

Kulsi, Goutam ; Sannigrahi, Achinta ; Mishra, Snehasis ; Das Saha, Krishna ; Datta, Sriparna ; Chattopadhyay, Partha ; Chattopadhyay, Krishnananda (2020) A novel cyclic mobile transporter can induce apoptosis by facilitating chloride anion transport into cells ACS Omega, 5 (27). pp. 16395-16405. ISSN 2470-1343

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Official URL: http://doi.org/10.1021/acsomega.0c00438

Related URL: http://dx.doi.org/10.1021/acsomega.0c00438

Abstract

We report here the preparation of an aminoxy amide-based pseudopeptide-derived building block using furanoid sugar molecules. Through the cyclo-oligomerization reaction, we generate a hybrid triazole/aminoxy amide macrocycle using the as-prepared building block. The novel conformation of the macrocycle has been characterized using NMR and molecular modeling studies, which show a strong resemblance of our synthesized compound to d-,l-α-aminoxy acid-based cyclic peptides that contain uniform backbone chirality. We observe that the macrocycle can efficiently and selectively bind Cl– ion and transport Cl– ion across a lipid bilayer. 1H NMR anion binding studies suggest a coherent relationship between the acidity of aminoxy amide N–H and triazole C–H proton binding strength. Using time-based fluorescence assay, we show that the macrocycle acts as a mobile transporter and follows an antiport mechanism. Our synthesized macrocycle imposes cancer cell death by disrupting ionic homeostasis through Cl– ion transport. The macrocycle induced cytochrome c leakage and changes in mitochondrial membrane potential along with activation of family of caspases, suggesting that the cellular apoptosis occurs through a caspase-dependent intrinsic pathway. The present results suggest the possibility of using the macrocycle as a biological tool of high therapeutic value.

Item Type:Article
Source:Copyright of this article belongs to American Chemical Society.
ID Code:137162
Deposited On:02 Sep 2025 08:23
Last Modified:02 Sep 2025 08:23

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