Microscale Thermophoresis and Molecular Modelling to Explore the Chelating Drug Transportation in the Milk to Infant

Mufarreh Asmari; Muhammad Waqas; Adel Ehab Ibrahim; Sobia Ahsan Halim; Ajmal Khan; Ahmed Al-Harrasi; Hermann Wätzig; Sami El Deeb

doi:10.3390/molecules27144604

Microscale Thermophoresis and Molecular Modelling to Explore the Chelating Drug Transportation in the Milk to Infant

Molecules. 2022 Jul 19;27(14):4604. doi: 10.3390/molecules27144604.

Authors

Mufarreh Asmari¹, Muhammad Waqas², Adel Ehab Ibrahim^{2

3}, Sobia Ahsan Halim², Ajmal Khan², Ahmed Al-Harrasi², Hermann Wätzig⁴, Sami El Deeb^{2

4}

Affiliations

¹ College of Pharmacy, King Khalid University, Abha 62529, Saudi Arabia.
² Natural and Medical Sciences Research Center, University of Nizwa, P.O. Box 33, Birkat Al Mauz, Nizwa 616, Oman.
³ Analytical Chemistry Department, Faculty of Pharmacy, Port-Said University, Port Fouad 42526, Egypt.
⁴ Institute of Medicinal and Pharmaceutical Chemistry, Technische Universität Braunschweig, 38106 Braunschweig, Germany.

Abstract

The microscale thermophoresis (MST) technique was utilized to investigate lactoferrin-drug interaction with the iron chelator, deferiprone, using label-free system. MST depends on the intrinsic fluorescence of one interacting partner. The results indicated a significant interaction between lactoferrin and deferiprone. The estimated binding constant for the lactoferrin-deferiprone interaction was 8.9 × 10^-6 ± 1.6, SD, which is to be reported for the first time. Such significant binding between lactoferrin and deferiprone may indicate the potentiation of the drug secretion into a lactating mother's milk. The technique showed a fast and simple approach to study protein-drug interaction while avoiding complicated labeling procedures. Moreover, the binding behavior of deferiprone within the binding sites of lactoferrin was investigated through molecular docking which reflected that deferiprone mediates strong hydrogen bonding with ARG121 and ASP297 in pocket 1 and forms H-bond and ionic interaction with ASN640 and ASP395, respectively, in pocket 2 of lactoferrin. Meanwhile, iron ions provide ionic interaction with deferiprone in both of the pockets. The molecular dynamic simulation further confirmed that the binding of deferiprone with lactoferrin brings conformational changes in lactoferrin that is more energetically stable. It also confirmed that deferiprone causes positive correlation motion in the interacting residues of both pockets, with strong negative correlation motion in the loop regions, and thus changes the dynamics of lactoferrin. The MM-GBSA based binding free energy calculation revealed that deferiprone exhibits ∆G TOTAL of -63,163 kcal/mol in pocket 1 and -63,073 kcal/mol in pocket 2 with complex receptor-ligand difference in pocket 1 and pocket 2 of -117.38 kcal/mol and -111.54 kcal/mol, respectively, which in turn suggests that deferiprone binds more strongly in the pocket 1. The free energy landscape of the lactoferrin-deferiprone complex also showed that this complex remains in a high energy state that confirms the strong binding of deferiprone with the lactoferrin. The current research concluded that iron-chelating drugs (deferiprone) can be transported from the mother to the infant in the milk because of the strong attachment with the lactoferrin active pockets.

Keywords: deferiprone; dissociation constant; lactoferrin; microscale thermophoresis; molecular modeling.

MeSH terms

Deferiprone
Female
Humans
Lactation
Lactoferrin*
Milk, Human*
Molecular Docking Simulation
Molecular Dynamics Simulation

Substances

Deferiprone
Lactoferrin

Grants and funding

This research received no external funding.