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Cofas Vargas L. F., Olivos-Ramirez G. E., Chwastyk M.♦, Moreira R.A.♦, Baker J. L.♦, Marrink S. J.♦, Poma Bernaola A.M., Nanomechanical footprint of SARS-CoV-2 variants in complex with a potent nanobody by molecular simulations,
NANOSCALE, ISSN: 2040-3364, DOI: 10.1039/D4NR02074J, Vol.16, No.40, pp.18824-18834, 2024Streszczenie: Rational design of novel antibody therapeutics against viral infections such as coronavirus relies on surface complementarity and high affinity for their effectiveness. Here, we explore an additional property of protein complexes, the intrinsic mechanical stability, in SARS-CoV-2 variants when complexed with a potent antibody. In this study, we utilized a recent implementation of the GōMartini 3 approach to investigate large conformational changes in protein complexes with a focus on the mechanostability of the receptor-binding domain (RBD) from WT, Alpha, Delta, and XBB.1.5 variants in complex with the H11-H4 nanobody. The analysis revealed moderate differences in mechanical stability among these variants. Also, we identified crucial residues in both the RBD and certain protein segments in the nanobody that contribute to this property. By performing pulling simulations and monitoring the presence of specific native and non-native contacts across the protein complex interface, we provided mechanistic insights into the dissociation process. Force-displacement profiles indicate a tensile force clamp mechanism associated with the type of protein complex. Our computational approach not only highlights the key mechanostable interactions that are necessary to maintain overall stability, but it also paves the way for the rational design of potent antibodies that are mechanostable and effective against emergent SARS-CoV-2 variants. Słowa kluczowe: SARS-CoV-2, GōMartini 3, Nanomechanics, Protein complexes, protein engineering, MD, native contacts Afiliacje autorów:
Cofas Vargas L. F. | - | IPPT PAN | Olivos-Ramirez G. E. | - | IPPT PAN | Chwastyk M. | - | Institute of Physics, Polish Academy of Sciences (PL) | Moreira R.A. | - | inna afiliacja | Baker J. L. | - | The College of New Jersey (US) | Marrink S. J. | - | inna afiliacja | Poma Bernaola A.M. | - | IPPT PAN |
| | 140p. |
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Moreira R., Vargas Guzman H.♦, Boopathi S.♦, Baker J.L.♦, Poma Bernaola A., Characterization of structural and energetic differences between conformations of the SARS-CoV-2 spike protein,
Materials, ISSN: 1996-1944, DOI: 10.3390/ma13235362, Vol.13, No.23, pp.5362-1-14, 2020Streszczenie: The novel coronavirus disease 2019 (COVID-19) pandemic has disrupted modern societies and their economies. The resurgence in COVID-19 cases as part of the second wave is observed across Europe and the Americas. The scientific response has enabled a complete structural characterization of the Severe Acute Respiratory Syndrome—novel Coronavirus 2 (SARS-CoV-2). Among the most relevant proteins required by the novel coronavirus to facilitate the cell entry mechanism is the spike protein. This protein possesses a receptor-binding domain (RBD) that binds the cellular angiotensin-converting enzyme 2 (ACE2) and then triggers the fusion of viral and host cell membranes. In this regard, a comprehensive characterization of the structural stability of the spike protein is a crucial step to find new therapeutics to interrupt the process of recognition. On the other hand, it has been suggested that the participation of more than one RBD is a possible mechanism to enhance cell entry. Here, we discuss the protein structural stability based on the computational determination of the dynamic contact map and the energetic difference of the spike protein conformations via the mapping of the hydration free energy by the Poisson–Boltzmann method. We expect our result to foster the discussion of the number of RBD involved during recognition and the repurposing of new drugs to disable the recognition by discovering new hotspots for drug targets apart from the flexible loop in the RBD that binds the ACE2. Słowa kluczowe: COVID-19, SARS-CoV-2, spike protein, RBD, structural stability, large conformational changes, protein complexes, free energy, molecular dynamics, dynamics contact analysis Afiliacje autorów:
Moreira R. | - | IPPT PAN | Vargas Guzman H. | - | Max-Planck-Institute for Polymer Research (DE) | Boopathi S. | - | inna afiliacja | Baker J.L. | - | The College of New Jersey (US) | Poma Bernaola A. | - | IPPT PAN |
| | 140p. |
3. |
Moreira R., Chwastyk M.♦, Baker J.L.♦, Vargas Guzman H.A.♦, Poma A., Quantitative determination of mechanical stability in the novel coronavirus spike protein,
NANOSCALE, ISSN: 2040-3364, DOI: 10.1039/D0NR03969A, Vol.12, No.31, pp.16409-16413, 2020Streszczenie: We report on the novel observation about the gain in mechanical stability of the SARS-CoV-2 (CoV2) spike (S) protein in comparison with SARS-CoV from 2002 (CoV1). Our findings have several biological implications in the subfamily of coronaviruses, as they suggest that the receptor binding domain (RBD) (~200 amino acids) plays a fundamental role as a damping element of the massive viral particle's motion prior to cell-recognition, while also facilitating viral attachment, fusion and entry. The mechanical stability via pulling of the RBD is 250 pN and 200 pN for CoV2 and CoV1 respectively, and the additional stability observed for CoV2 (~50 pN) might play a role in the increasing spread of COVID-19. Afiliacje autorów:
Moreira R. | - | IPPT PAN | Chwastyk M. | - | Institute of Physics, Polish Academy of Sciences (PL) | Baker J.L. | - | The College of New Jersey (US) | Vargas Guzman H.A. | - | Max-Planck-Institute for Polymer Research (DE) | Poma A. | - | IPPT PAN |
| | 140p. |