Epitope characterization and crystal structure of GA101 provide insights into the molecular basis for type I/II distinction of CD20 antibodies.

نویسندگان

  • Gerhard Niederfellner
  • Alfred Lammens
  • Olaf Mundigl
  • Guy J Georges
  • Wolfgang Schaefer
  • Manfred Schwaiger
  • Andreas Franke
  • Kornelius Wiechmann
  • Stefan Jenewein
  • Jerry W Slootstra
  • Peter Timmerman
  • Annika Brännström
  • Frida Lindstrom
  • Ekkehard Mössner
  • Pablo Umana
  • Karl-Peter Hopfner
  • Christian Klein
چکیده

CD20 is a cell-surface marker of normal and malignant B cells. Rituximab, a monoclonal antibody targeting CD20, has improved the treatment of malignant lymphomas. Therapeutic CD20 antibodies are classified as either type I or II based on different mechanisms of killing malignant B cells. To reveal the molecular basis of this distinction, we fine-mapped the epitopes recognized by both types. We also determined the first X-ray structure of a type II antibody by crystallizing the obinutuzumab (GA101) Fab fragment alone and in complex with a CD20 cyclopeptide. Despite recognizing an overlapping epitope, GA101 binds CD20 in a completely different orientation than type I antibodies. Moreover, the elbow angle of GA101 is almost 30° wider than in type I antibodies, potentially resulting in different spatial arrangements of 2 CD20 molecules bound to a single GA101 or rituximab molecule. Using protein tomography, different CD20 complexes were found to be associated with the 2 antibodies, and confocal microscopy showed different membrane compartmentalization of these subpopulations of the cellular CD20 pool. Our findings offer a possible molecular explanation for the different cellular responses elicited by type I and II antibodies.

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عنوان ژورنال:
  • Blood

دوره 118 2  شماره 

صفحات  -

تاریخ انتشار 2011