Abstract
Human biospecimen collection, processing and preservation are rapidly emerging subjects providing essential support to clinical as well as basic researchers. Unlike collection of other biospecimens (e.g. DNA and serum), biobanking of viable immune cells, such as peripheral blood mononuclear cells (PBMC) and/or isolated immune cell subsets is still in its infancy. While certain aspects of processing and freezing conditions have been studied in the past years, little is known about the effect of blood transportation on immune cell survival, phenotype and specific functions. However, especially for multicentric and cooperative projects it is vital to precisely know those effects. In this study we investigated the effect of blood shipping and pre-processing delay on immune cell phenotype and function both on cellular and subcellular levels. Peripheral blood was collected from healthy volunteers (n = 9): at a distal location (shipped overnight) and in the central laboratory (processed immediately). PBMC were processed in the central laboratory and analyzed post-cryopreservation. We analyzed yield, major immune subset distribution, proliferative capacity of T cells, cytokine pattern and T-cell receptor signal transduction. Results show that overnight transportation of blood samples does not globally compromise T- cell subsets as they largely retain their phenotype and proliferative capacity. However, NK and B cell frequencies, the production of certain PBMC-derived cytokines and IL-6 mediated cytokine signaling pathway are altered due to transportation. Various control experiments have been carried out to compare issues related to shipping versus pre-processing delay on site. Our results suggest the implementation of appropriate controls when using multicenter logistics for blood transportation aiming at subsequent isolation of viable immune cells, e.g. in multicenter clinical trials or studies analyzing immune cells/subsets. One important conclusion might be that despite changes due to overnight shipment, highly standardized central processing (and analysis) could be superior to multicentric de-central processing with more difficult standardization.
Highlights
Characterization and analysis of human blood and immune cell phenotype and function is becoming more and more important both for experimental and clinical studies: among others, this is relevant to investigating the mechanisms of action of immune therapies, monitoring immune function or addressing basic scientific questions related to the etiopathogenesis of various diseases and/or their therapeutic targeting
Before investigating the effect of shipping on blood samples we ran a comparative test of different blood sampling tubes on the overall peripheral blood mononuclear cells (PBMC) yield
First we investigated the effects of blood transportation on PBMC yield and viability
Summary
Characterization and analysis of human blood and immune cell phenotype and function is becoming more and more important both for experimental and clinical studies: among others, this is relevant to investigating the mechanisms of action of immune therapies, monitoring immune function or addressing basic scientific questions related to the etiopathogenesis of various diseases and/or their therapeutic targeting. Analysis of peripheral immune response is essential for assessing response patterns and better understanding treatment and/or diseaseinduced immunological effects and immune competence, as well as for validating the clinical relevance of newly discovered biomarkers. All these aspects require high quality blood samples allowing isolation of viable and functionally unaltered immune cells for further experimental analysis to make precise observations and thereby reliable conclusions. Likewise, centralized biobank facilities specialized for biospecimen collection, ensure controlled transport, cryopreservation, and regular quality assessment of collected biospecimen and thereby guarantee good quality biomaterial benefiting both clinical and basic researchers
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