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The clearance kinetics of autologous RhD-positive erythrocytes coated ex vivo with novel recombinant and monoclonal anti-D antibodies

  1. G. E. Chapman1,
  2. J. R. Ballinger2,
  3. M. J. Norton1,
  4. D. R. Parry-Jones2,
  5. N. A. Beharry2,
  6. C. Cousins3,
  7. C. H. Dash1,
  8. A. M. Peters2,*

Article first published online: 3 AUG 2007

DOI: 10.1111/j.1365-2249.2007.03458.x

Issue

Clinical & Experimental Immunology

Clinical & Experimental Immunology

Volume 150, Issue 1, pages 30–41, October 2007

Additional Information

How to Cite

Chapman, G. E., Ballinger, J. R., Norton, M. J., Parry-Jones, D. R., Beharry, N. A., Cousins, C., Dash, C. H. and Peters, A. M. (2007), The clearance kinetics of autologous RhD-positive erythrocytes coated ex vivo with novel recombinant and monoclonal anti-D antibodies. Clinical & Experimental Immunology, 150: 30–41. doi: 10.1111/j.1365-2249.2007.03458.x

Author Information

  1. 1

    Bio Products Laboratory, Elstree, Hertfordshire, and Departments of

  2. 2

    Nuclear Medicine and

  3. 3

    Radiology, Addenbrooke's Hospital, Cambridge, UK

*Professor a m. Peters, Brighton Sussex Medical School, Audrey Emerton Building, Royal Sussex County Hospital, Eastern Road, Brighton BN2 5BE, UK. E-mail: a.m.peters@bsms.ac.uk

Publication History

  1. Issue published online: 3 AUG 2007
  2. Article first published online: 3 AUG 2007
  3. Accepted for publication 4 June 2007

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Keywords:

  • antibodies;
  • Fc receptors;
  • human;
  • red cell clearance;
  • RhD antigen

Summary

Anti-D is given routinely to pregnant RhD-negative women to prevent haemolytic disease of the fetus and newborn. To overcome the potential drawbacks associated with plasma-derived products, monoclonal and recombinant forms of anti-D have been developed. The ability of two such antibodies, BRAD-3/5 monoclonal anti-D IgG (MAD) and rBRAD-3/5 recombinant anti-D IgG (RAD), to clear RhD-positive erythrocytes from the circulation was compared using a dual radiolabelling technique. Six RhD-positive males received autologous erythrocytes radiolabelled with 99mTc and 51Cr and coated ex vivo with MAD and RAD. Blood samples were collected up to 1 h following intravenous injection, and percentage dose of radioactivity in the samples determined. Three different levels of coating were used on three separate occasions. No significant differences between MAD and RAD were observed in the initial clearance rate constant at any dose level. The log[activity]-time clearance plots were curved, showing a reduction in the clearance rate constant with time. This reduction was more marked for RAD than for MAD. The results support a dynamic model for the clearance of antibody-coated erythrocytes that may have wider relevance for the therapeutic use of antibodies.

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