3mwq Citations

Crystal structure of RNase A tandem enzymes and their interaction with the cytosolic ribonuclease inhibitor.

Arnold U, Leich F, Neumann P, Lilie H, Ulbrich-Hofmann R
FEBS J 278 331-40 (2011)
Related entries: 3mwr, 3mx8

Cited: 9 times
EuropePMC logo PMID: 21134128

Abstract

Because of their ability to degrade RNA, RNases are potent cytotoxins. The cytotoxic activity of most members of the RNase A superfamily, however, is abolished by the cytosolic ribonuclease inhibitor (RI). RNase A tandem enzymes, in which two RNase A molecules are artificially connected by a peptide linker, and thus have a pseudodimeric structure, exhibit remarkable cytotoxic activity. In vitro, however, these enzymes are still inhibited by RI. Here, we present the crystal structures of three tandem enzymes with the linker sequences GPPG, SGSGSG, and SGRSGRSG, which allowed us to analyze the mode of binding of RI to the RNase A tandem enzymes. Modeling studies with the crystal structures of the RI-RNase A complex and the SGRSGRSG-RNase A tandem enzyme as templates suggested a 1 : 1 binding stoichiometry for the RI-RNase A tandem enzyme complex, with binding of the RI molecule to the N-terminal RNase A entity. These results were experimentally verified by analytical ultracentrifugation, quantitative electrophoresis, and proteolysis studies with trypsin. As other dimeric RNases, which are comparably cytotoxic, either evade RI binding or potentially even bind two RI molecules, inactivation by RI cannot be the crucial limitation to the cytotoxicity of dimeric RNases.

Articles - 3mwq mentioned but not cited (1)

  1. Improving protocols for protein mapping through proper comparison to crystallography data. Lexa KW, Carlson HA. J Chem Inf Model 53 391-402 (2013)


Reviews citing this publication (2)

  1. Biological Activities of Secretory RNases: Focus on Their Oligomerization to Design Antitumor Drugs. Gotte G, Menegazzi M. Front Immunol 10 2626 (2019)
  2. Structural and functional relationships of natural and artificial dimeric bovine ribonucleases: new scaffolds for potential antitumor drugs. Gotte G, Laurents DV, Merlino A, Picone D, Spadaccini R. FEBS Lett 587 3601-3608 (2013)

Articles citing this publication (6)

  1. Rational design and evaluation of mammalian ribonuclease cytotoxins. Lomax JE, Eller CH, Raines RT. Methods Enzymol 502 273-290 (2012)
  2. An endogenous ribonuclease inhibitor regulates the antimicrobial activity of ribonuclease 7 in the human urinary tract. Spencer JD, Schwaderer AL, Eichler T, Wang H, Kline J, Justice SS, Cohen DM, Hains DS. Kidney Int 85 1179-1191 (2014)
  3. New insight into secreted ribonuclease structure: binase is a natural dimer. Dudkina E, Kayumov A, Ulyanova V, Ilinskaya O. PLoS One 9 e115818 (2014)
  4. Regulation of IRE1 RNase activity by the Ribonuclease inhibitor 1 (RNH1). Tavernier Q, Bennana E, Poindessous V, Schaeffer C, Rampoldi L, Pietrancosta N, Pallet N. Cell Cycle 17 1901-1916 (2018)
  5. RNase A Domain-Swapped Dimers Produced Through Different Methods: Structure-Catalytic Properties and Antitumor Activity. Montioli R, Campagnari R, Fasoli S, Fagagnini A, Caloiu A, Smania M, Menegazzi M, Gotte G. Life (Basel) 11 168 (2021)
  6. Incorporation of extra amino acids in peptide recognition probe to improve specificity and selectivity of an electrochemical peptide-based sensor. Zaitouna AJ, Maben AJ, Lai RY. Anal Chim Acta 886 157-164 (2015)


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