Abstract

CHI currently manages 26 active collaborations across 8 Institutes and the Clinical Center. These are divided into 3 stages: sample collection (8 studies), assay (9 studies), and write up (9 studies). An example is the CHAPLE study with Mike Lenardo, where a cohort of longitudinally sampled children with CD55 deficiency have been treated with eculizumab, a substitute complement inhibitor. CHI has performed SomaLogic analysis of peripheral blood serum, finding between cases and controls 96 proteins which differ significantly (FDR<0.05) prior to therapy, of which 36 proteins change significantly in cases within 1 week of therapy. Ongoing work will involve CyTOF phenotyping of PBL, in addition to stool microbiome analysis. This represents a study where high dimensional phenotyping can lead to better understanding of the patient pathology, may inform use of a nascent therapy, and give basic biology insight into, in this case, CD55 function and the mechanisms of complement inhibition. CHI also provides fee-for-service access to assays not otherwise accessible to NIH reseachers. The SomaLogic proteomic assay has been run for over 3000 samples, for 7 investigators, in the last year. To develop this capacity, a 35 marker mass cytometry immune phenotyping assay and analysis pipeline has been adapted for fee-for service deployment. To support CHIs mission we continue to develop infrastructure. For single cell sequencing technologies using the 10x plaform, we have developed CITE-Seq analysis and TCR sequencing. With mass cytometry, an assay has been established to quantify phosphorylation of 10 intracellular proteins, in addition to 20 cell phenotype markers, in response to 12 in vitro stimulation conditions. For flow cytometry, we have validated a 28 color cytometry panel on a new BD FACSymphony, and onboarded a spectral sorter. Throughout we are optimizing automation technologies, such as for cell staining (Tecan Fluent) and NGS library preparation (pipeline of QIAsymphony, Biomek FX, Agilent TapeStation and QIAgility). Going forward we are testing O-link as replacement for SomaLogic serum proteomic analysis, and exploring isolation and analysis of leukocytes from tissues.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Scientific Cores Intramural Research (ZIC)
Project #
1ZICAI001226-02
Application #
10015019
Study Section
Project Start
Project End
Budget Start
Budget End
Support Year
2
Fiscal Year
2019
Total Cost
Indirect Cost

  Institution

Name
National Institute of Allergy and Infectious Diseases
Department
Type
DUNS #
City
State
Country
Zip Code

  Publications

Giudice, Valentina; Wu, Zhijie; Kajigaya, Sachiko et al. (2018) Circulating S100A8 and S100A9 protein levels in plasma of patients with acquired aplastic anemia and myelodysplastic syndromes. Cytokine :
El-Chemaly, Souheil; Cheung, Foo; Kotliarov, Yuri et al. (2018) The Immunome in Two Inherited Forms of Pulmonary Fibrosis. Front Immunol 9:76
Tanaka, Toshiko; Biancotto, Angelique; Moaddel, Ruin et al. (2018) Plasma proteomic signature of age in healthy humans. Aging Cell 17:e12799
Chen, Jinguo; Cheung, Foo; Shi, Rongye et al. (2018) PBMC fixation and processing for Chromium single-cell RNA sequencing. J Transl Med 16:198
Elinoff, Jason M; Chen, Li-Yuan; Dougherty, Edward J et al. (2018) Spironolactone-induced degradation of the TFIIH core complex XPB subunit suppresses NF-?B and AP-1 signalling. Cardiovasc Res 114:65-76
Sanchez, Gina A Montealegre; Reinhardt, Adam; Ramsey, Suzanne et al. (2018) JAK1/2 inhibition with baricitinib in the treatment of autoinflammatory interferonopathies. J Clin Invest 128:3041-3052
Ou, Jingxing; Ball, John M; Luan, Yizhao et al. (2018) iPSCs from a Hibernator Provide a Platform for Studying Cold Adaptation and Its Potential Medical Applications. Cell 173:851-863.e16
Candia, Julián; Cheung, Foo; Kotliarov, Yuri et al. (2017) Assessment of Variability in the SOMAscan Assay. Sci Rep 7:14248
Hosokawa, Kohei; Kajigaya, Sachiko; Keyvanfar, Keyvan et al. (2017) Whole transcriptome sequencing identifies increased CXCR2 expression in PNH granulocytes. Br J Haematol 177:136-141
Giudice, Valentina; Feng, Xingmin; Kajigaya, Sachiko et al. (2017) Optimization and standardization of fluorescent cell barcoding for multiplexed flow cytometric phenotyping. Cytometry A 91:694-703

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