Sodium Thiosulphate-Loaded Liposomes Control Hydrogen Sulphide Release and Retain Its Biological Properties in Hypoxia-like Environment

Lissette Sanchez-Aranguren; Milda Grubliauskiene; Hala Shokr; Pavanjeeth Balakrishnan; Keqing Wang; Shakil Ahmad; Mandeep Kaur Marwah

doi:10.3390/antiox11112092

Sodium Thiosulphate-Loaded Liposomes Control Hydrogen Sulphide Release and Retain Its Biological Properties in Hypoxia-like Environment

Antioxidants (Basel). 2022 Oct 24;11(11):2092. doi: 10.3390/antiox11112092.

Authors

Lissette Sanchez-Aranguren¹, Milda Grubliauskiene^{1

2}, Hala Shokr³, Pavanjeeth Balakrishnan⁴, Keqing Wang¹, Shakil Ahmad¹, Mandeep Kaur Marwah¹

Affiliations

¹ Aston Medical School, College of Health and Life Sciences, Aston University, Birmingham B4 7ET, UK.
² Mirzyme Therapeutics, Innovation Birmingham Campus, Faraday Wharf, Holt Street, Birmingham B7 4BB, UK.
³ Pharmacy Division, School of Health Sciences, Faculty of Biology, Medicine and Health, University of Manchester, Manchester M13 9PL, UK.
⁴ School of Engineering and Technology, College of Engineering and Physical Sciences, Aston University, Birmingham B4 7ET, UK.

Abstract

Hypoxia, or insufficient oxygen availability is a common feature in the development of a myriad of cardiovascular-related conditions including ischemic disease. Hydrogen sulphide (H₂S) donors, such as sodium thiosulphate (STS), are known for their cardioprotective properties. However, H₂S due to its gaseous nature, is released and cleared rapidly, limiting its potential translation to clinical settings. For the first time, we developed and characterised liposome formulations encapsulating STS and explored their potential for modulating STS uptake, H₂S release and the ability to retain pro-angiogenic and biological signals in a hypoxia-like environment mirroring oxygen insufficiency in vitro. Liposomes were prepared by varying lipid ratios and characterised for size, polydispersity and charge. STS liposomal encapsulation was confirmed by HPLC-UV detection and STS uptake and H₂S release was assessed in vitro. To mimic hypoxia, cobalt chloride (CoCl₂) was administered in conjunction with formulated and non-formulated STS, to explore pro-angiogenic and metabolic signals. Optimised liposomal formulation observed a liposome diameter of 146.42 ± 7.34 nm, a polydispersity of 0.22 ± 0.19, and charge of 3.02 ± 1.44 mV, resulting in 25% STS encapsulation. Maximum STS uptake (76.96 ± 3.08%) from liposome encapsulated STS was determined at 24 h. Co-exposure with CoCl₂ and liposome encapsulated STS resulted in increased vascular endothelial growth factor mRNA as well as protein expression, enhanced wound closure and increased capillary-like formation. Finally, liposomal STS reversed metabolic switch induced by hypoxia by enhancing mitochondrial bioenergetics. These novel findings provide evidence of a feasible controlled-delivery system for STS, thus H₂S, using liposome-based nanoparticles. Likewise, data suggests that in scenarios of hypoxia, liposomal STS is a good therapeutic candidate to sustain pro-angiogenic signals and retain metabolic functions that might be impaired by limited oxygen and nutrient availability.

Keywords: angiogenesis; controlled-release; drug delivery systems; hydrogen sulphide; liposomes; mitochondrial metabolism.

Grants and funding

RGS\R1\221169/Royal Society