FFA4 has gained interest in recent years since its deorphanization in 2005 and the characterization of the Free Fatty Acids receptors family for their therapeutic potential in metabolic disorders. The expression of FFA4 (also known as GPR120) in numerous organs throughout the human body makes this receptor a highly potent target, particularly in fat sensing and diet preference. This offers an attractive approach to tackle obesity and related metabolic diseases. Recent cryo-EM structures of the receptor have provided valuable information for a potential active state although the previous studies of FFA4 presented diverging information. We performed molecular docking and molecular dynamics simulations of four agonist ligands, TUG-891, Linoleic acid, alpha-Linolenic acid, and Oleic acid, based on a homology model. Our simulations, which accumulated a total of 2 mu s of simulation, highlighted two binding hotspots at Arg992.64 and Lys293 (ECL3). The results indicate that the residues are located in separate areas of the binding pocket and interact with various types of ligands, implying different potential active states of FFA4 and a highly adaptable binding intra-receptor pocket. This article proposes additional structural characteristics and mechanisms for agonist binding that complement the experimental structures. Homology modeling of Free Fatty Acid receptor 4 (FFA4) and molecular dynamics of agonists-FFA4 complexes have shown a new binding hotspot, Lys293, and revealed a different binding preference for Lys293 or the already known Arg99 between synthetic or natural ligands. image
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Natl Dong Hwa Univ, Dept Life Sci, Hualien, Taiwan
Natl Dong Hwa Univ, Inst Biotechnol, Hualien, TaiwanXiamen Med Coll, Ctr Transit Med, Dept Basic Med Sci, Xiamen 361023, Fujian, Peoples R China
Chang, Chia-Hsiang
Tsai, May-Jwan
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Taipei Vet Gen Hosp, Neurol Inst, Neural Regenerat Lab, Taipei, TaiwanXiamen Med Coll, Ctr Transit Med, Dept Basic Med Sci, Xiamen 361023, Fujian, Peoples R China
Tsai, May-Jwan
Cheng, Henrich
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Taipei Vet Gen Hosp, Neurol Inst, Neural Regenerat Lab, Taipei, TaiwanXiamen Med Coll, Ctr Transit Med, Dept Basic Med Sci, Xiamen 361023, Fujian, Peoples R China
Cheng, Henrich
Chen, Jian-Chyi
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Southern Taiwan Univ Sci & Technol, Dept Biotechnol, Tainan, TaiwanXiamen Med Coll, Ctr Transit Med, Dept Basic Med Sci, Xiamen 361023, Fujian, Peoples R China
Chen, Jian-Chyi
Leong, Max K.
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Natl Dong Hwa Univ, Dept Chem, 1,Sec 2,Da Hsueh Rd, Hualien 97401, TaiwanXiamen Med Coll, Ctr Transit Med, Dept Basic Med Sci, Xiamen 361023, Fujian, Peoples R China
Leong, Max K.
Weng, Ching-Feng
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Xiamen Med Coll, Ctr Transit Med, Dept Basic Med Sci, Xiamen 361023, Fujian, Peoples R ChinaXiamen Med Coll, Ctr Transit Med, Dept Basic Med Sci, Xiamen 361023, Fujian, Peoples R China
机构:
Yeungnam Univ, Dept Med Biotechnol, 280 Daehak Ro, Gyongsan 38541, Gyeongbuk, South KoreaYeungnam Univ, Dept Med Biotechnol, 280 Daehak Ro, Gyongsan 38541, Gyeongbuk, South Korea
Baig, Mohammad Hassan
Rahman, Safikur
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Yeungnam Univ, Dept Med Biotechnol, 280 Daehak Ro, Gyongsan 38541, Gyeongbuk, South KoreaYeungnam Univ, Dept Med Biotechnol, 280 Daehak Ro, Gyongsan 38541, Gyeongbuk, South Korea
Rahman, Safikur
Rabbani, Gulam
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Yeungnam Univ, Dept Med Biotechnol, 280 Daehak Ro, Gyongsan 38541, Gyeongbuk, South KoreaYeungnam Univ, Dept Med Biotechnol, 280 Daehak Ro, Gyongsan 38541, Gyeongbuk, South Korea
Rabbani, Gulam
Imran, Mohd
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All India Inst Med Sci, Dept Biophys, New Delhi 110029, IndiaYeungnam Univ, Dept Med Biotechnol, 280 Daehak Ro, Gyongsan 38541, Gyeongbuk, South Korea
Imran, Mohd
Ahmad, Khurshid
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Yeungnam Univ, Dept Med Biotechnol, 280 Daehak Ro, Gyongsan 38541, Gyeongbuk, South KoreaYeungnam Univ, Dept Med Biotechnol, 280 Daehak Ro, Gyongsan 38541, Gyeongbuk, South Korea
Ahmad, Khurshid
Choi, Inho
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Yeungnam Univ, Dept Med Biotechnol, 280 Daehak Ro, Gyongsan 38541, Gyeongbuk, South KoreaYeungnam Univ, Dept Med Biotechnol, 280 Daehak Ro, Gyongsan 38541, Gyeongbuk, South Korea