[HTML][HTML] Forecasting the cytokine storm following systemic interleukin (IL)-2 administration
MC Panelli, R White, M Foster, B Martin… - Journal of translational …, 2004 - Springer
MC Panelli, R White, M Foster, B Martin, E Wang, K Smith, FM Marincola
Journal of translational medicine, 2004•SpringerExtensive clinical experience has shown that systemic interleukin (IL)-2 administration can
induce complete or partial regression of renal cell cancer (RCC) metastases in 15 to 20% of
patients. Since IL-2 has no direct anti-cancer effects, it is believed that cancer regression is
mediated either by a direct modulation of immune cell effector functions or through the
mediation of soluble factors released as a result of IL-2 administration. We previously
observed that transcriptional and protein changes induced by systemic IL-2 administration …
induce complete or partial regression of renal cell cancer (RCC) metastases in 15 to 20% of
patients. Since IL-2 has no direct anti-cancer effects, it is believed that cancer regression is
mediated either by a direct modulation of immune cell effector functions or through the
mediation of soluble factors released as a result of IL-2 administration. We previously
observed that transcriptional and protein changes induced by systemic IL-2 administration …
Abstract
Extensive clinical experience has shown that systemic interleukin (IL)-2 administration can induce complete or partial regression of renal cell cancer (RCC) metastases in 15 to 20 % of patients. Since IL-2 has no direct anti-cancer effects, it is believed that cancer regression is mediated either by a direct modulation of immune cell effector functions or through the mediation of soluble factors released as a result of IL-2 administration.
We previously observed that transcriptional and protein changes induced by systemic IL-2 administration affect predominantly mononuclear phagocytes with little effect, particularly within the tumor microenvironment, on T cell activation, localization and proliferation. It further appeared that mononuclear phagocyte activation could be best explained by the indirect mediation of a secondary release of cytokines by IL-2 responsive cells either in the circulation or in peripheral tissues.
To better characterize the cytokine outburst that follows systemic IL-2 administration we followed the serum levels of 68 soluble factors in ten patients with RCC undergoing high dose (720,000 IU/kg intravenously every 8 hours) IL-2 therapy. Serum was collected before therapy, 3 hours after the 1st and 4th dose and assayed on a multiplexed protein array platform. This study demonstrated that 1) the serum concentration of more than half the soluble factors studied changed significantly during therapy; 2) changes became more dramatic with increasing doses; 3) subclasses of soluble factors displayed different kinetics and 4) cytokine patterns varied quantitatively among patients.
This study shows that the cytokine storm that follows systemic IL-2 administration is complex and far-reaching inclusive of soluble factors with disparate, partly redundant and partly contrasting effects on immune function. Therefore comparing in parallel large number of soluble factors, it sets a comprehensive foundation for further elucidation of "cytokine storm" in larger patient pools. Based on this analysis, we propose a prospective collection of serum samples in a larger cohort of patients undergoing IL-2 administration with the purpose of discerning patterns predictive of clinical outcome and toxicity.
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