A new methodology for polyvalent intravenous immunoglobulin solution production with a two-stage process of viral inactivation

Authors

  • Antônio Edson de Souza Lucena University of Pernambuco; Department of Pharmaceutical Sciences Federal
  • Divaldo de Almeida Sampaio Federal University of Pernambuco; Department of Clinical Medicine
  • Ednaldo Rosas da Silva Healt Bureau of Pernambuco State Government; Foundation of Pernambuco
  • Virgínia Florêncio de Paiva Healt Bureau of Pernambuco State Government; Foundation of Pernambuco
  • Ana Cláudia Santiago Healt Bureau of Pernambuco State Government; Foundation of Pernambuco
  • Ana Cristina Lima Leite Healt Bureau of Pernambuco State Government; Foundation of Pernambuco

DOI:

https://doi.org/10.1590/S1984-82502010000400020

Keywords:

Blood derivatives, Immunoglobulins, Polyethylene glycol, Ultrafiltration, Ion exchange chromatography

Abstract

Highly purified intravenous immunoglobulin G concentrate (IV IgG) was produced with the use of polyethylene glycol associated to a single-stage precipitation by ethanol, instead of the classic Cohn-Oncley process, which employs cold alcohol as the precipitating agent, in a three-stage process. Precipitation of crude fraction containing more than 95% of immunoglobulin G was performed by liquid chromatography with a cation exchanger, CM-Sepharose, as a stationary phase. During the process, the product was subjected to two-stage viral inactivation. The first stage was performed by the action of sodium caprylate, 30 mM at pH 5.1+/- 0.1, and the second stage was performed by the action of a solvent-detergent mixture. The finished product was formulated at 5% with 10% sucralose as the stabilizing agent. The process yields 3.3g of IgG/liter of plasma. The finished product analysis showed an anti-complementary activity lower than 1CH50. Polymer and aggregate percent levels were lower than 3% in the five batches studied. The analysis of neutralizing capacity showed the presence of antibacterial and antiviral antibodies in at least three times higher concentrations than the levels found in source plasma. The finished product fulfilled all purity requirements stated in the 4th edition of the European pharmacopeia.

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Published

2010-12-01

Issue

Vol. 46 No. 4 (2010)

Section

Articles

License

All content of the journal, except where identified, is licensed under a Creative Commons attribution-type BY.

The on line journal has open and free access.

How to Cite

A new methodology for polyvalent intravenous immunoglobulin solution production with a two-stage process of viral inactivation . (2010). Brazilian Journal of Pharmaceutical Sciences, 46(4), 777-783. https://doi.org/10.1590/S1984-82502010000400020