Polybetaine nanobrushes are widely used as inert platforms for label-free biosensing due to their resistance to nonspecific interactions. Despite being considered cationic or electrically neutral, polybetaines can exhibit a negative zeta potential (ZP) at pHs above their isoelectric point (pI). To clarify whether negative zeta potential effectively contributes to surface interactions, we examined three types of nanobrushes deposited on a planar gold substrate: two polybetaines: poly(carboxybetaine methacrylamide) (pCBMAA) and poly(sulfobetaine methacrylamide) (pSBMAA) and hydrophilic poly[N-(2-hydroxypropyl) methacrylamide] (pHPMAA), which carries no ionic group. All three brushes exhibit a well-defined pI and negative surface ZP at pHs above their pI. The pH dependence of the interactions of these brushes with anionic dextran sulfate (DS) and cationic poly[(N-trimethylammonium)ethyl methacrylate] (PTMAEMA) was monitored by infrared reflection spectroscopies (infrared reflection absorption spectroscopy (IRRAS), grazing angle attenuated total reflectance (GAATR)). DS adsorbs to pCBMAA strongly and only weakly to pSBMAA at pHs below their pI but can adsorb slightly to both polybetaines even at pHs above their pI. This is due to the displacement of their carboxylate or sulfo groups from the interaction with the quaternary ammonium cation by the DS sulfate groups. However, DS does not adsorb to pHPMAA at any pH, and PTMAEMA does not adsorb to any of the brushes, regardless of pH. These findings highlight that zeta potential determinations alone may not be sufficient to predict electrostatic interactions as the apparent negative charge does not necessarily translate into a functional surface charge influencing macromolecular interactions.

• Publikační typ
• časopisecké články MeSH

Antibiotic-resistant strains of Staphylococcus aureus pose a significant threat in healthcare, demanding urgent therapeutic solutions. Combining bacteriophages with conventional antibiotics, an innovative approach termed phage-antibiotic synergy, presents a promising treatment avenue. However, to enable new treatment strategies, there is a pressing need for methods to assess their efficacy reliably and rapidly. Here, we introduce a novel approach for real-time monitoring of pathogen lysis dynamics employing the piezoelectric quartz crystal microbalance (QCM) with dissipation (QCM-D) technique. The sensor, a QCM chip modified with the bacterium S. aureus RN4220 ΔtarM, was utilized to monitor the activity of the enzyme lysostaphin and the phage P68 as model lytic agents. Unlike conventional QCM solely measuring resonance frequency changes, our study demonstrates that dissipation monitoring enables differentiation of bacterial growth and lysis caused by cell-attached lytic agents. Compared to reference turbidimetry measurements, our results reveal distinct alterations in the growth curve of the bacteria adhered to the sensor, characterized by a delayed lag phase. Furthermore, the dissipation signal analysis facilitated the precise real-time monitoring of phage-mediated lysis. Finally, the QCM-D biosensor was employed to evaluate the synergistic effect of subinhibitory concentrations of the antibiotic amoxicillin with the bacteriophage P68, enabling monitoring of the lysis of P68-resistant wild-type strain S. aureus RN4220. Our findings suggest that this synergy also impedes the formation of bacterial aggregates, the precursors of biofilm formation. Overall, this method brings new insights into phage-antibiotic synergy, underpinning it as a promising strategy against antibiotic-resistant bacterial strains with broad implications for treatment and prevention.

• Klíčová slova
• Staphylococcus aureus, Antimicrobial treatment, Multidrug-resistant bacteria, Phage therapy, Phage-antibiotic synergy, Piezoelectric biosensor,
• MeSH
• antibakteriální látky farmakologie   MeSH
• bakteriofágy fyziologie   MeSH
• bakteriolýza * účinky léků   MeSH
• biosenzitivní techniky * metody   přístrojové vybavení   MeSH
• lysostafin farmakologie   MeSH
• mikrorovnovážné techniky křemenného krystalu * metody   MeSH
• Staphylococcus aureus * účinky léků   virologie   růst a vývoj   MeSH
• Publikační typ
• časopisecké články MeSH
• práce podpořená grantem MeSH
• Názvy látek
• antibakteriální látky MeSH
• lysostafin MeSH