Expression, purification and crystallization of CTB-MPR, a candidate mucosal vaccine component against HIV-1

نویسندگان

  • Ho-Hsien Lee
  • Irene Cherni
  • HongQi Yu
  • Raimund Fromme
  • Jeffrey D. Doran
  • Ingo Grotjohann
  • Michele Mittman
  • Shibom Basu
  • Arpan Deb
  • Katerina Dörner
  • Andrew Aquila
  • Anton Barty
  • Sébastien Boutet
  • Henry N. Chapman
  • R. Bruce Doak
  • Mark S. Hunter
  • Daniel James
  • Richard A. Kirian
  • Christopher Kupitz
  • Robert M. Lawrence
  • Haiguang Liu
  • Karol Nass
  • Ilme Schlichting
  • Kevin E. Schmidt
  • M. Marvin Seibert
  • Robert L. Shoeman
  • John C. H. Spence
  • Francesco Stellato
  • Uwe Weierstall
  • Garth J. Williams
  • Chunhong Yoon
  • Dingjie Wang
  • Nadia A. Zatsepin
  • Brenda G. Hogue
  • Nobuyuki Matoba
  • Petra Fromme
  • Tsafrir S. Mor
چکیده

CTB-MPR is a fusion protein between the B subunit of cholera toxin (CTB) and the membrane-proximal region of gp41 (MPR), the transmembrane envelope protein of Human immunodeficiency virus 1 (HIV-1), and has previously been shown to induce the production of anti-HIV-1 antibodies with antiviral functions. To further improve the design of this candidate vaccine, X-ray crystallography experiments were performed to obtain structural information about this fusion protein. Several variants of CTB-MPR were designed, constructed and recombinantly expressed in Escherichia coli. The first variant contained a flexible GPGP linker between CTB and MPR, and yielded crystals that diffracted to a resolution of 2.3 Å, but only the CTB region was detected in the electron-density map. A second variant, in which the CTB was directly attached to MPR, was shown to destabilize pentamer formation. A third construct containing a polyalanine linker between CTB and MPR proved to stabilize the pentameric form of the protein during purification. The purification procedure was shown to produce a homogeneously pure and monodisperse sample for crystallization. Initial crystallization experiments led to pseudo-crystals which were ordered in only two dimensions and were disordered in the third dimension. Nanocrystals obtained using the same precipitant showed promising X-ray diffraction to 5 Å resolution in femtosecond nanocrystallography experiments at the Linac Coherent Light Source at the SLAC National Accelerator Laboratory. The results demonstrate the utility of femtosecond X-ray crystallography to enable structural analysis based on nano/microcrystals of a protein for which no macroscopic crystals ordered in three dimensions have been observed before.

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عنوان ژورنال:

دوره 1  شماره 

صفحات  -

تاریخ انتشار 2014