Crystal Structure of the Herpes Simplex Virus

نویسندگان

  • Shenping Liu
  • John D. Knafels
  • Jeanne S. Chang
  • Gregory A. Waszak
  • Eric T. Baldwin
  • Martin R. Deibel
  • Darrell R. Thomsen
  • Fred L. Homa
  • Peter A. Wells
  • Monica C. Tory
  • Roger A. Poorman
  • Hua Gao
  • Xiayang Qiu
  • Andrew P. Seddon
چکیده

Herpesviruses are the second leading cause of human viral diseases. Herpes SimplexVirus types 1 and 2 andVaricella-zoster virus produce neurotropic infections such as cutaneous and genital herpes, chickenpox, and shingles. Infections of a lymphotropic nature are caused by cytomegalovirus, HSV-6, HSV-7, and Epstein-Barr virus producing lymphoma, carcinoma, and congenital abnormalities. Yet another series of serious health problems are posed by infections in immunocompromised individuals. Common therapies for herpes viral infections employ nucleoside analogs, such as Acyclovir, and target the viral DNApolymerase, essential for viral DNA replication. Although clinically useful, this class of drugs exhibits a narrow antiviral spectrum, and resistance to these agents is an emergingproblem for diseasemanagement.Abetter understanding of herpes virus replicationwill help thedevelopment of new safe and effective broad spectrum anti-herpetic drugs that fill an unmet need. Here, we present the first crystal structure of a herpesvirus polymerase, the Herpes Simplex Virus type 1 DNA polymerase, at 2.7 Å resolution. The structural similarity of this polymerase to other polymerases has allowed us to construct high confidence models of a replication complex of the polymerase and of Acyclovir as a DNA chain terminator. We propose a novel inhibition mechanism in which a representative of a series of non-nucleosidic viral polymerase inhibitors, the 4-oxo-dihydroquinolines, binds at the polymerase active site interacting non-covalently with both the polymerase and the DNA duplex.

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تاریخ انتشار 2006