Implementation of Highly Sophisticated Flow Cytometry Assays in Multicenter Clinical Studies: Considerations and Guidance

Sommer, Ulrike; Morales, Johanna K.; Groenewegen, A.; Müller, Alfons; Naab, Julia; Woerly, G.; Kamphausen, Esther; Marsot, Helene; Bennett, Patrick; Kakkanaiah, Vellalore N.; Vitaliti, Alessandra

doi:10.4155/bio.15.61

Cited by 10 publications

(16 citation statements)

References 40 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…For the TVT, its utility has already been described in this fashion in publications such as Poirier et al (9) and Sommer et al (14). Regression analysis results showed that there was only one case where the correlation coefficient (r value) failed to meet the ≥0.90 target (TVT vs BD = 0.89 for CD16/56 on Day 11) for both devices.…”

Section: While There Have Been Comparative Studies Between the Transfmentioning

confidence: 80%

“…These results highlight that both devices can be used in a capacity where a centralized analysis laboratory for immunophenotyping is required for clinical development purposes. For the TVT, its utility has already been described in this fashion in publications such as Poirier et al (9) and Sommer et al (14).…”

Section: While There Have Been Comparative Studies Between the Transfmentioning

confidence: 99%

See 1 more Smart Citation

Interlaboratory comparison of the TransFix®/EDTA Vacuum Blood Collection tube with the 5 mL Cyto‐Chex® BCT

Harrison¹,

Ward

Bastow

et al. 2018

Cytometry Part B Clinical

View full text Add to dashboard Cite

Background: An interlaboratory study was performed to compare the performance of the 3 mL TransFix ® / EDTA Vacuum Blood Collection Tube (TVT), with the 5 mL Cyto-Chex ® BCT tube (BCT). Both devices are intended for collection and storage of whole blood specimens for immunophenotyping of leukocytes by flow cytometry for up to 14 days.Methods: One site in the United States and two in the United Kingdom tested samples from 10 HIV positive patients and four healthy subjects for a total of 42 samples. From each subject, three blood samples were collected: a BD 4 mL K 3 EDTA Vacutainer (Vacutainer), a TVT, and a BCT. At all sites, samples were analyzed on a BD FACS Canto II flow cytometer for a full lymphocyte subset count within 6 h of collection (all devices) and on Day 11 and Day 15 (TVT and BCT only). Data obtained from the Vacutainer were used as the control data set with which TVT and BCT data were statistically compared.Results and Conclusions: Statistical concordance was demonstrated for both devices in relation to cell absolute count recovery. For cell marker signal, both devices exhibited a significant decrease in mean fluorescence intensity (MFI) for the detection of lymphocyte subsets and their target markers. There was a marked increase in autofluorescence observed for BCT stabilized lymphocytes whereas values for the TVTs were comparable to the control. There were eight instances of statistical equivalence between the level of antibody autofluorescence observed in the control tube and the TVT across both patient cohorts, versus two for the BCT.

show abstract

Section: While There Have Been Comparative Studies Between the Transfmentioning

confidence: 80%

Section: While There Have Been Comparative Studies Between the Transfmentioning

confidence: 99%

Interlaboratory comparison of the TransFix®/EDTA Vacuum Blood Collection tube with the 5 mL Cyto‐Chex® BCT

Harrison¹,

Ward

Bastow

et al. 2018

Cytometry Part B Clinical

View full text Add to dashboard Cite

show abstract

“…Several variables such as sample/specimen choice and preparation, instruments setup and alignment, and data acquisition and analysis impact the outcome and reliability of large scale multicenter studies involving FCM; as identified by the survey and the live discussions. The main outcomes and suggestions from the WS were: Control of sample stability (from few hours to several days) is a critical factor in choosing a distributed processing approach and several methods to enhance sample stability are well documented and should be consulted . Lab‐to‐lab variations in sample processing and analyses were considered major sources of data variability resulting from subjective analyses along with the potential variability introduced by the use of multiple instruments and operators. The need for access to disease‐state samples for use in assay development and as control material. Suitable samples could come from commercial vendors, clinical partner networks, or the creation of biobanks of disease samples. …”

Section: Discussionmentioning

confidence: 99%

“…• Control of sample stability (from few hours to several days) is a critical factor in choosing a distributed processing approach and several methods to enhance sample stability are well documented and should be consulted (93,94). • Lab-to-lab variations in sample processing and analyses were considered major sources of data variability resulting from subjective analyses along with the potential variability introduced by the use of multiple instruments and operators.…”

Section: Discussionmentioning

confidence: 99%

“…Additional samples need to be included as controls both for the stimulation and for correct gating of the population of interest . Shipping of a sample to a central lab for inducible biomarker testing presents an additional challenge in that even though the cells' immunophenotypes do not change, their ability to respond to a stimulus might be compromised due to travel .…”

Section: Ws12: Inducible Biomarkersmentioning

confidence: 99%

See 1 more Smart Citation

Cyt‐Geist: Current and Future Challenges in Cytometry: Reports of the CYTO 2018 Conference Workshops

Czechowska¹,

Lannigan

Wang

et al. 2019

Cytometry Pt A

Self Cite

View full text Add to dashboard Cite

Flow cytometric method transfer: Recommendations for best practice

Cabanski

Oldaker²,

Stewart

et al. 2020

Cytometry Part B Clinical

Self Cite

View full text Add to dashboard Cite

As with many aspects of the validation and monitoring of flow cytometric methods, the method transfer processes and acceptance criteria described for other technologies are not fully applicable. This is due to the complexity of the highly configurable instrumentation, the complexity of cellular measurands, the lack of qualified reference materials for most assays, and limited specimen stability. There are multiple reasons for initiating a method transfer, multiple regulatory settings, and multiple context of use. All of these factors influence the specific requirements for the method transfer. This recommendation paper describes the considerations and best practices for the transfer of flow cytometric methods and provides individual case studies as examples. In addition, the manuscript emphasizes the importance of appropriately conducting a method transfer on data reliability.

show abstract

Implementation of Highly Sophisticated Flow Cytometry Assays in Multicenter Clinical Studies: Considerations and Guidance

Cited by 10 publications

References 40 publications

Interlaboratory comparison of the TransFix®/EDTA Vacuum Blood Collection tube with the 5 mL Cyto‐Chex® BCT

Interlaboratory comparison of the TransFix®/EDTA Vacuum Blood Collection tube with the 5 mL Cyto‐Chex® BCT

Cyt‐Geist: Current and Future Challenges in Cytometry: Reports of the CYTO 2018 Conference Workshops

Flow cytometric method transfer: Recommendations for best practice

Contact Info

Product

Resources

About