User:Carson Powers/Sandbox 1

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Another mini protein inhibitor, <scene name='10/1076041/Lcb3_only/3'>LCB3,</scene> was developed using the same computational method as LCB1 and binds to the same region of the RBD, except in the opposite direction. Its <scene name='10/1076041/Lcb3xspikecorlabel_intxn/1'>binding interactions</scene> also show a large number of hydrogen bonds. However, LCB1 has more surface area and fits more precisely with its computational model, giving it a slightly higher binding affinity.
Another mini protein inhibitor, <scene name='10/1076041/Lcb3_only/3'>LCB3,</scene> was developed using the same computational method as LCB1 and binds to the same region of the RBD, except in the opposite direction. Its <scene name='10/1076041/Lcb3xspikecorlabel_intxn/1'>binding interactions</scene> also show a large number of hydrogen bonds. However, LCB1 has more surface area and fits more precisely with its computational model, giving it a slightly higher binding affinity.
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The LCBs have a significantly higher affinity for the spike RBD and are smaller and more stable than traditional antibodies. Their reduced size allows these molecules to tightly pack more interactions in the active site as well as improve their ability to enter the respiratory system.
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==Significance==
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The designed mini protein inhibitors have a significantly higher affinity for the spike protein compared to the ACE2 receptor, especially the LCBs. [[Image:Kd_table.png|200px|right|Table 1. Dissociation constants (Kd) in nM for SARS-CoV-2 spike RBD binding to ACE2 and engineered minibinders, measured by biolayer interferometry to compare affinities for the spike protein.]] The LCBs have a significantly higher affinity for the spike RBD and are smaller and more stable than traditional antibodies. Their reduced size allows these molecules to tightly pack more interactions in the active site as well as improve their ability to enter the respiratory system.
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==Significance==
 
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The designed mini protein inhibitors have a significantly higher affinity for the spike protein compared to the ACE2 receptor, especially the LCBs. [[Image:Kd_table.png|200px|right|Table 1. Dissociation constants (Kd) in nM for SARS-CoV-2 spike RBD binding to ACE2 and engineered minibinders, measured by biolayer interferometry to compare affinities for the spike protein.]]
 

Revision as of 14:57, 26 April 2025

De novo miniprotein Covid therapeutic

LCB1 bound to spike protein. LCB1 is colored pink and shown in cartoon. The spike protein is colored by chain and shown by its surface. PDB file: 7jzl

Drag the structure with the mouse to rotate

References

Proteopedia Page Contributors and Editors (what is this?)

Carson Powers

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