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   in-silico investigation of the erbb family dimerization mechanism  
   
نویسنده mashayekh poul romina ,azimzadeh irani maryam ,masoomi nomandan zeinab
منبع رياضيات زيستي - 1401 - دوره : 4 - ریاضیات زیستی - کد همایش: 01220-42743 - صفحه:0 -0
چکیده    The human epidermal growth factor receptor family contains four distinct receptors,including erbb1, erbb2, erbb3, and erbb4. these receptors are the key players of cellsignaling in tumor development and function in heterodimer or homodimer forms. this studyexplores the erbb hetero and homodimers’ potential in constructing the active back-to-backdimer using molecular modeling and molecular docking techniques. among the modeleddimers, 21 out of 37 back-to-back ones were heterodimers. suggesting that heterodimerizationis the dominant active form of the erbb receptors. docking results show that erbb1-erbb1,erbb1-erbb4, and erbb2-erbb3 dimers are the most favorable dimeric structures.these findings are crucial in defining novel epitopes for therapeutic anti-cancer designs againsterbb receptors.
کلیدواژه erbb receptors ,heterodimerization ,homodimerization ,molecular docking
آدرس , iran, , iran, , iran
 
     
   
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