Influence of the Human Parainfluenza Virus 3 Attachment Protein's Neuraminidase Activity on Its Capacity To Activate the Fusion Protein

doi:10.1128/JVI.79.4.2383-2392.2005

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Journal of Virology, February 2005, p. 2383-2392, Vol. 79, No. 4
0022-538X/05/$08.00+0 doi:10.1128/JVI.79.4.2383-2392.2005
Copyright © 2005, American Society for Microbiology. All Rights Reserved.

Influence of the Human Parainfluenza Virus 3 Attachment Protein's Neuraminidase Activity on Its Capacity To Activate the Fusion Protein

Matteo Porotto,¹ Matthew Murrell,¹ Olga Greengard,¹ Lynne Doctor,¹ and Anne Moscona¹^*

Department of Pediatrics, Mount Sinai School of Medicine, New York, New York¹

Received 13 August 2004/ Accepted 30 September 2004

In order to examine functions of the hemagglutinin-neuraminidase(HN) protein that quantitatively influence fusion promotion,human parainfluenza virus 3 (HPIV3) variants with alterationsin HN were studied. The variant HNs have mutations that affecteither receptor binding avidity, neuraminidase activity, orfusion protein (F) activation. Neuraminidase activity was regulatedby manipulation of temperature and pH. F activation was assessedby quantitating the irreversible binding of target erythrocytes(RBC) to HN/F-coexpressing cells in the presence of 4-GU-DANA(zanamivir) to release target cells bound only by HN-receptorinteractions; the remaining, irreversibly bound target cellsare retained via the fusion protein. In cells coexpressing wild-type(wt) or variant HNs with wt F, the fusion promotion capacityof HN was distinguished from target cell binding by measuringchanges with time in the amounts of target RBC that were (i)reversibly bound by HN-receptor interaction (released only uponthe addition of 4-GU-DANA), (ii) released by HN's neuraminidase,and (iii) irreversibly bound by F-insertion or fusion (F triggered).For wt HN, lowering the pH (to approach the optimum for HPIV3neuraminidase) decreased F triggering via release of HN fromits receptor. An HN variant with increased receptor bindingavidity had F-triggering efficiency like that of wt HN at pH8.0, but this efficiency was not decreased by lowering the pHto 5.7, which suggested that the variant HN's higher receptorbinding activity counterbalanced the receptor dissociation promotedby increased neuraminidase activity. To dissect the specificcontribution of neuraminidase to triggering, two variant HNsthat are triggering-defective due to a mutation in the HN stalkwere evaluated. One of these variants has, in addition, a mutationin the globular head that renders it neuraminidase dead, whilethe HN with the stalk mutation alone has 30% of wt neuraminidase.While the variant without neuraminidase activity triggered Feffectively at 37°C irrespective of pH, the variant possessingeffective neuraminidase activity completely failed to activateF at pH 5.7 and was capable of only minimal triggering activityeven at pH 8.0. These results demonstrate that neuraminidaseactivity impacts the extent of HPIV3-mediated fusion by releasingHN from contact with receptor. Any particular HN's competenceto promote F-mediated fusion depends on the balance betweenits inherent F-triggering efficacy and its receptor-attachmentregulatory functions (binding and receptor cleavage).

* Department of Pediatrics, Mount Sinai School of Medicine, 1 Gustave L. Levy Pl., New York, NY 10029. Phone: (212) 241-9709. Fax: (212) 860-3316. E-mail: anne.moscona{at}mssm.edu.

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