Your search keyword '"David J.H.F. Knapp"' showing total 69 results

1. UM171 Enhances Lentiviral Gene Transfer and Recovery of Primitive Human Hematopoietic Cells

Author

Mor Ngom, Suzan Imren, Tobias Maetzig, Jennifer E. Adair, David J.H.F. Knapp, Jalila Chagraoui, Iman Fares, Marie-Eve Bordeleau, Guy Sauvageau, Philippe Leboulch, Connie Eaves, and Richard Keith Humphries

Subjects

Genetics, QH426-470, Cytology, QH573-671

Abstract

Enhanced gene transfer efficiencies and higher yields of transplantable transduced human hematopoietic stem cells are continuing goals for improving clinical protocols that use stemcell-based gene therapies. Here, we examined the effect of the HSC agonist UM171 on these endpoints in both in vitro and in vivo systems. Using a 22-hr transduction protocol, we found that UM171 significantly enhances both the lentivirus-mediated transduction and yield of CD34+ and CD34+CD45RA- hematopoietic cells from human cord blood to give a 6-fold overall higher recovery of transduced hematopoietic stem cells, including cells with long-term lympho-myeloid repopulating activity in immunodeficient mice. The ability of UM171 to enhance gene transfer to primitive cord blood hematopoietic cells extended to multiple lentiviral pseudotypes, gamma retroviruses, and non-integrating lentiviruses and to adult bone marrow cells. UM171, thus, provides an interesting reagent for improving the ex vivo production of gene-modified cells and for reducing requirements of virus for a broad range of applications. Keywords: lentivirus, gene transfer, hematopoietic stem cells

Published

2018

2. High-Resolution Single-Cell DNA Methylation Measurements Reveal Epigenetically Distinct Hematopoietic Stem Cell Subpopulations

Author

Tony Hui, Qi Cao, Joanna Wegrzyn-Woltosz, Kieran O'Neill, Colin A. Hammond, David J.H.F. Knapp, Emma Laks, Michelle Moksa, Samuel Aparicio, Connie J. Eaves, Aly Karsan, and Martin Hirst

Subjects

Medicine (General), R5-920, Biology (General), QH301-705.5

Abstract

Summary: Increasing evidence of functional and transcriptional heterogeneity in phenotypically similar cells examined individually has prompted interest in obtaining parallel methylome data. We describe the development and application of such a protocol to index-sorted murine and human hematopoietic cells that are highly enriched in their content of functionally defined stem cells. Utilizing an optimized single-cell bisulfite sequencing protocol, we obtained quantitative DNA methylation measurements of up to 5.7 million CpGs in single hematopoietic cells. In parallel, we developed an analytical strategy (PDclust) to define single-cell DNA methylation states through pairwise comparisons of single-CpG methylation measurements. PDclust revealed that a single-cell epigenetic state can be described by a small (

Published

2018

3. Mass Cytometric Analysis Reveals Viable Activated Caspase-3+ Luminal Progenitors in the Normal Adult Human Mammary Gland

Author

David J.H.F. Knapp, Nagarajan Kannan, Davide Pellacani, and Connie J. Eaves

Subjects

Biology (General), QH301-705.5

Abstract

Summary: The normal adult human female mammary gland is a bilayered structure consisting of an outer basal layer and two readily distinguished subsets of cells within the inner luminal layer. We now present a validated methodology for undertaking large-scale multi-parameter mass cytometric analyses of these cell types at single-cell resolution. In addition, we show how combining this approach with in vitro clonogenic assays of the proliferative and signaling responses of normal human mammary cells to epidermal growth factor (EGF) allows additional subsets with different EGF responses to be discerned. This included the identification of a subset of cells within the phenotypically defined luminal progenitor fraction that displays an elevated content of active caspase-3, including some that generate clones in vitro in response to EGF, with immunohistochemical evidence of their presence in situ in fixed preparations of normal human breast tissue. : Knapp et al. identify a subpopulation of progenitors in the human mammary gland that have partially activated an apoptotic program despite retaining some viability and clonogenic potential. As such activation has been linked to genomic instability, these cells may be at increased risk for oncogenic transformation. Keywords: mammary, mass cytometry, cancer, apoptosis, signaling, cell death, genomic instability, single-cell biology, growth factors

Published

2017

4. A Dominant-Negative Isoform of IKAROS Expands Primitive Normal Human Hematopoietic Cells

Author

Philip A. Beer, David J.H.F. Knapp, Nagarajan Kannan, Paul H. Miller, Sonja Babovic, Elizabeth Bulaeva, Nima Aghaeepour, Gabrielle Rabu, Shabnam Rostamirad, Kingsley Shih, Lisa Wei, and Connie J. Eaves

Subjects

Medicine (General), R5-920, Biology (General), QH301-705.5

Abstract

Disrupted IKAROS activity is a recurrent feature of some human leukemias, but effects on normal human hematopoietic cells are largely unknown. Here, we used lentivirally mediated expression of a dominant-negative isoform of IKAROS (IK6) to block normal IKAROS activity in primitive human cord blood cells and their progeny. This produced a marked (10-fold) increase in serially transplantable multipotent IK6+ cells as well as increased outputs of normally differentiating B cells and granulocytes in transplanted immunodeficient mice, without producing leukemia. Accompanying T/natural killer (NK) cell outputs were unaltered, and erythroid and platelet production was reduced. Mechanistically, IK6 specifically increased human granulopoietic progenitor sensitivity to two growth factors and activated CREB and its targets (c-FOS and Cyclin B1). In more primitive human cells, IK6 prematurely initiated a B cell transcriptional program without affecting the hematopoietic stem cell-associated gene expression profile. Some of these effects were species specific, thus identifying novel roles of IKAROS in regulating normal human hematopoietic cells.

Published

2014

5. Distinct Stromal Cell Factor Combinations Can Separately Control Hematopoietic Stem Cell Survival, Proliferation, and Self-Renewal

Author

Stefan Wohrer, David J.H.F. Knapp, Michael R. Copley, Claudia Benz, David G. Kent, Keegan Rowe, Sonja Babovic, Heidi Mader, Robert A.J. Oostendorp, and Connie J. Eaves

Subjects

Biology (General), QH301-705.5

Abstract

Hematopoietic stem cells (HSCs) are identified by their ability to sustain prolonged blood cell production in vivo, although recent evidence suggests that durable self-renewal (DSR) is shared by HSC subtypes with distinct self-perpetuating differentiation programs. Net expansions of DSR-HSCs occur in vivo, but molecularly defined conditions that support similar responses in vitro are lacking. We hypothesized that this might require a combination of factors that differentially promote HSC viability, proliferation, and self-renewal. We now demonstrate that HSC survival and maintenance of DSR potential are variably supported by different Steel factor (SF)-containing cocktails with similar HSC-mitogenic activities. In addition, stromal cells produce other factors, including nerve growth factor and collagen 1, that can antagonize the apoptosis of initially quiescent adult HSCs and, in combination with SF and interleukin-11, produce >15-fold net expansions of DSR-HSCs ex vivo within 7 days. These findings point to the molecular basis of HSC control and expansion.

Published

2014

6. The miR-185/PAK6 axis predicts therapy response and regulates survival of drug-resistant leukemic stem cells in CML

Author

Katharina Rothe, Artem Babaian, Keith Keith Humphries, Jonathan Zeng, Xiaoyan Jiang, Min Chen, Donna L. Forrest, Hanyang Lin, Oleh Petriv, Inanc Birol, Connie J. Eaves, Jens Ruschmann, Tobias Maetzig, Ryan R. Brinkman, David J.H.F. Knapp, Naoto Nakamichi, Kieran O'Neill, Carl L. Hansen, Ryan Yen, and Andrew Wu

Subjects

0301 basic medicine, MAPK/ERK pathway, Xenotransplantation, medicine.medical_treatment, Immunology, Mice, SCID, Drug resistance, Biology, Biochemistry, Mice, 03 medical and health sciences, 0302 clinical medicine, Cancer stem cell, Leukemia, Myelogenous, Chronic, BCR-ABL Positive, microRNA, medicine, Animals, Humans, Progenitor cell, Protein Kinase Inhibitors, Myeloid Neoplasia, Gene Expression Regulation, Leukemic, Myeloid leukemia, Cell Biology, Hematology, MicroRNAs, 030104 developmental biology, p21-Activated Kinases, Drug Resistance, Neoplasm, 030220 oncology & carcinogenesis, Neoplastic Stem Cells, Cancer research, Heterografts, Stem cell, Signal Transduction

Abstract

Overcoming drug resistance and targeting cancer stem cells remain challenges for curative cancer treatment. To investigate the role of microRNAs (miRNAs) in regulating drug resistance and leukemic stem cell (LSC) fate, we performed global transcriptome profiling in treatment-naive chronic myeloid leukemia (CML) stem/progenitor cells and identified that miR-185 levels anticipate their response to ABL tyrosine kinase inhibitors (TKIs). miR-185 functions as a tumor suppressor: its restored expression impaired survival of drug-resistant cells, sensitized them to TKIs in vitro, and markedly eliminated long-term repopulating LSCs and infiltrating blast cells, conferring a survival advantage in preclinical xenotransplantation models. Integrative analysis with mRNA profiles uncovered PAK6 as a crucial target of miR-185, and pharmacological inhibition of PAK6 perturbed the RAS/MAPK pathway and mitochondrial activity, sensitizing therapy-resistant cells to TKIs. Thus, miR-185 presents as a potential predictive biomarker, and dual targeting of miR-185-mediated PAK6 activity and BCR-ABL1 may provide a valuable strategy for overcoming drug resistance in patients.

Published

2020

7. Survey Says: 'COVID-19 Lockdown Hits Young Faculty and Clinical Trials'

Author

David G. Kent, David J.H.F. Knapp, and Nagarajan Kannan

Subjects

0301 basic medicine, 2019-20 coronavirus outbreak, medicine.medical_specialty, Biomedical Research, Coronavirus disease 2019 (COVID-19), Pneumonia, Viral, education, MEDLINE, Biology, Biochemistry, Article, 03 medical and health sciences, 0302 clinical medicine, Surveys and Questionnaires, Genetics, medicine, Humans, Laboratory research, Intensive care medicine, Pandemics, health care economics and organizations, Clinical Trials as Topic, COVID-19, Cell Biology, medicine.disease, Research Personnel, Clinical trial, Pneumonia, 030104 developmental biology, Stem cell, Coronavirus Infections, 030217 neurology & neurosurgery, Developmental Biology

Abstract

COVID-19 has severely impacted laboratory research. Analysis of the International Society for Stem Cell Research (ISSCR) member survey has highlighted a particular impact on clinical trials and early-career investigators. The stem cell community needs to support young researchers and ensure that stem cell medicine does not lose its momentum.

Published

2020

8. Altered microRNA expression links IL6 and TNF-induced inflammaging with myeloid malignancy in humans and mice

Author

Aparna Gopal, Megan Fuller, Yu Deng, Mark Boldin, Jennifer M Grants, Aly Karsan, Joanna Wegrzyn, David J.H.F. Knapp, Connie J. Eaves, T. Roderick Docking, Tony Hui, Jenny Li, Marion Shadbolt, Kieran O'Neill, Jeremy Parker, and Martin Hirst

Subjects

Adult, Male, Aging, Myeloid, Adolescent, Immunology, Inflammation, Biochemistry, Mice, Young Adult, microRNA, medicine, Animals, Humans, Cell Self Renewal, Interleukin 6, Cellular Senescence, Aged, Mice, Knockout, biology, Interleukin-6, Tumor Necrosis Factor-alpha, NF-kappa B, Hematopoietic stem cell, Cell Differentiation, Cell Biology, Hematology, DNA Methylation, Middle Aged, Hematopoietic Stem Cells, Leukemia, Myeloid, Acute, MicroRNAs, Haematopoiesis, medicine.anatomical_structure, DNA methylation, biology.protein, Cancer research, Cytokines, Female, Tumor necrosis factor alpha, Single-Cell Analysis, medicine.symptom, Transcriptome, BLOOD Commentary

Abstract

Aging is associated with significant changes in the hematopoietic system, including increased inflammation, impaired hematopoietic stem cell (HSC) function, and increased incidence of myeloid malignancy. Inflammation of aging (“inflammaging”) has been proposed as a driver of age-related changes in HSC function and myeloid malignancy, but mechanisms linking these phenomena remain poorly defined. We identified loss of miR-146a as driving aging-associated inflammation in AML patients. miR-146a expression declined in old wild-type mice, and loss of miR-146a promoted premature HSC aging and inflammation in young miR-146a–null mice, preceding development of aging-associated myeloid malignancy. Using single-cell assays of HSC quiescence, stemness, differentiation potential, and epigenetic state to probe HSC function and population structure, we found that loss of miR-146a depleted a subpopulation of primitive, quiescent HSCs. DNA methylation and transcriptome profiling implicated NF-κB, IL6, and TNF as potential drivers of HSC dysfunction, activating an inflammatory signaling relay promoting IL6 and TNF secretion from mature miR-146a−/− myeloid and lymphoid cells. Reducing inflammation by targeting Il6 or Tnf was sufficient to restore single-cell measures of miR-146a−/− HSC function and subpopulation structure and reduced the incidence of hematological malignancy in miR-146a−/− mice. miR-146a−/− HSCs exhibited enhanced sensitivity to IL6 stimulation, indicating that loss of miR-146a affects HSC function via both cell-extrinsic inflammatory signals and increased cell-intrinsic sensitivity to inflammation. Thus, loss of miR-146a regulates cell-extrinsic and -intrinsic mechanisms linking HSC inflammaging to the development of myeloid malignancy.

Published

2020

9. DLL4 and VCAM1 enhance the emergence of T cell-competent hematopoietic progenitors from human pluripotent stem cells

Author

C. Zimmerman, M. I. Ibanez-Rios, Y. S. Michaels, David J.H.F. Knapp, C. Lau, M. C. Major, Peter W. Zandstra, Ting Yin, E. L. Castle, A. Hagner, and J. M. Edgar

Subjects

biology, Chemistry, CD3, T cell, Notch signaling pathway, Acquired immune system, Cell biology, Haematopoiesis, medicine.anatomical_structure, biology.protein, medicine, Progenitor cell, Induced pluripotent stem cell, CD8

Abstract

T cells are key mediators of the adaptive immune response and show tremendous efficacy as cellular therapeutics. However, obtaining primary T cells from human donors is expensive and variable. Pluripotent stem cells (PSCs) have the potential to serve as a consistent and renewable source of T cells, but differentiating PSCs into hematopoietic progenitors with T cell potential remains a significant challenge. Here, we developed an efficient serum- and feeder-free protocol for differentiating human PSCs into hematopoietic progenitors and T cells. This defined method allowed us to study the impact of individual recombinant proteins on blood emergence and lineage potential. We demonstrate that the presence of DLL4 and VCAM1 during the endothelial-to-hematopoietic transition (EHT) enhances downstream progenitor T cell output by >80-fold. Using single cell transcriptomics, we showed that these two proteins synergise to drive strong notch signalling in nascent hematopoietic stem and progenitor cells and that VCAM1 additionally drives a pro-inflammatory transcriptional program. Finally, we applied this differentiation method to study the impact of cytokine concentration dynamics on T cell maturation. We established optimised media formulations that enabled efficient and chemically defined differentiation of CD8αβ+, CD4-, CD3+, TCRαβ+ T cells from PSCs.

Published

2021

10. Review of: 'Regulating expression of mistranslating tRNAs by readthrough RNA polymerase II transcription'

Author

David J.H.F. Knapp

Subjects

biology, Transcription (biology), biology.protein, RNA polymerase II, Cell biology

Published

2021

11. A topological view of human CD34+ cell state trajectories from integrated single-cell output and proteomic data

Author

Garry P. Nolan, Sean C. Bendall, Carl L. Hansen, Connie J. Eaves, Fangwu Wang, Michael VanInsberghe, Colin A. Hammond, Paul H. Miller, Davide Pellacani, Nima Aghaeepour, Philip A. Beer, and David J.H.F. Knapp

Subjects

0301 basic medicine, Lineage (genetic), Stromal cell, Cellular differentiation, Immunology, Cell Biology, Hematology, Biology, Topology, Biochemistry, 03 medical and health sciences, Haematopoiesis, 030104 developmental biology, 0302 clinical medicine, 030220 oncology & carcinogenesis, Cord blood, Compartment (development), Cell Cycle Protein, Transcription factor

Abstract

Recent advances in single-cell molecular analytical methods and clonal growth assays are enabling more refined models of human hematopoietic lineage restriction processes to be conceptualized. Here, we report the results of integrating single-cell proteome measurements with clonally determined lymphoid, neutrophilic/monocytic, and/or erythroid progeny outputs from >1000 index-sorted CD34+ human cord blood cells in short-term cultures with and without stromal cells. Surface phenotypes of functionally examined cells were individually mapped onto a molecular landscape of the entire CD34+ compartment constructed from single-cell mass cytometric measurements of 14 cell surface markers, 20 signaling/cell cycle proteins, and 6 transcription factors in ∼300 000 cells. This analysis showed that conventionally defined subsets of CD34+ cord blood cells are heterogeneous in their functional properties, transcription factor content, and signaling activities. Importantly, this molecular heterogeneity was reduced but not eliminated in phenotypes that were found to display highly restricted lineage outputs. Integration of the complete proteomic and functional data sets obtained revealed a continuous probabilistic topology of change that includes a multiplicity of lineage restriction trajectories. Each of these reflects progressive but variable changes in the levels of specific signaling intermediates and transcription factors but shared features of decreasing quiescence. Taken together, our results suggest a model in which increasingly narrowed hematopoietic output capabilities in neonatal CD34+ cord blood cells are determined by a history of external stimulation in combination with innately programmed cell state changes.

Published

2019

12. Barcoded Competitive Clone-Initiating Cell (BC-CIC) Analysis Reveals Differences in Ovarian Cancer Cell Genotype and Niche Specific Clonal Fitness During Growth and Metastasis In Vivo

Author

Upasana Ray, Jianning Song, David J.H.F. Knapp, Syed Mohammed Musheer Aalam, Jamie N. Bakkum-Gamez, Nagarajan Kannan, Xiaojia Tang, Viji Shridhar, Krishna R. Kalari, and Mark E. Sherman

Subjects

Cell, Clone (cell biology), Cancer, Computational biology, Biology, medicine.disease, medicine.disease_cause, Metastasis, medicine.anatomical_structure, Genotype, medicine, Ovarian cancer, Carcinogenesis, Gene

Abstract

During oncogenesis, pathogenic clones develop which contain cells capable of spreading throughout the body, ultimately compromising vital organ functions and physiology. Understanding how metastatic clones develop and spread is critical for improving cancer treatments. However, our understanding of these processes has been hampered by a paucity of quantitative methodologies to comprehensively map, track and characterize such clones. To address this shortcoming, we have developed a DNA barcoding and next-generation sequencing based system-wide clonal tracking technology integrated with a computational data analysis pipeline called Clone-Initiating Cell (CIC) Calculator. The CIC Calculator interfaces with the CIC Morbus Mandala (CIC-MM) plot, a novel tool to visually comprehend and detect four distinct categories that explains their complex relationships with various tissues/organ sites. Further, we describe machine learning approaches to study CIC number, frequency, and estimate clone size and distribution demonstrating distinct growth patterns, and their inter-relationships and their routes of metastatic spread at clonal resolution. We demonstrate these methodologies, using our novel multifunctional lentiviral barcode libraries, and specifically barcoded tubal-ovarian metastatic OVCAR5 cell lines (engineered to express varying levels of metastasis promoting LRRC15 gene) and co-injected cells in a competitive CIC assay into tubal or ovarian sites in highly immunodeficient NSG mice. DNA was isolated from primary tumors, omental/bowel metastasis and system-wide anatomical site/organs. Amplicon sequencing libraries were constructed with spike-in-control barcodes (serving as internal calibration controls) to estimate absolute clone sizes. The computational pipeline CIC Calculator was then used to deconvolute and filter the data, set stringent thresholds, and generate high-quality information on CIC numbers and frequencies, clone sizes, linkages across sites and classify clones based on their extent of metastatic activity. Using of CIC-MM plot, statistical models and machine learning approaches, we generated high-resolution clonal maps of metastasis for each animal. The information generated included clone types and system-wide metastasis, similar and dissimilar clonal patterns of dominance at heterotopic sites and their routes of metastases. The data revealed previously unknown influences of cellular genotype and their implanted sites on selecting certain clones with specific system-wide clonal patterns, and identified rare LRRC15 expressor clones (classified as CIC.Toti) predisposed to exploit ‘all’ sites, albeit at varying degrees of dominance. The genomic technology and computational methodology described here are tissue-agnostic. They enable rapid adoption for an investigation into various stages of system-wide metastasis and growth of transplantable malignant cells at the highest clonal resolution.

Published

2021

13. A blood transcriptome-based analysis of disease progression, immune regulation, and symptoms in coronavirus-infected patients

Author

Paschalis Vergidis, Nagarajan Kannan, Anguraj Sadanandam, Tobias Bopp, Krishnaraj Rajalingam, Alan Melcher, David J.H.F. Knapp, Santosh Dixit, and Chitra Priya Emperumal

Subjects

0301 basic medicine, Cancer Research, Molecular biology, medicine.medical_treatment, Immunology, Disease, medicine.disease_cause, lcsh:RC254-282, Peripheral blood mononuclear cell, Article, Transcriptome, 03 medical and health sciences, Cellular and Molecular Neuroscience, 0302 clinical medicine, Immunity, medicine, lcsh:QH573-671, B cell, Coronavirus, Innate immune system, lcsh:Cytology, business.industry, Cell Biology, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, 030104 developmental biology, medicine.anatomical_structure, Cytokine, 030220 oncology & carcinogenesis, business

Abstract

COVID-19 patients show heterogeneity in clinical presentation and outcomes that makes pandemic control and strategy difficult; optimizing management requires a systems biology approach of understanding the disease. Here we sought to potentially understand and infer complex disease progression, immune regulation, and symptoms in patients infected with coronaviruses (35 SARS-CoV and 3 SARS-CoV-2 patients and 57 samples) at two different disease progression stages. Further, we compared coronavirus data with healthy individuals (n = 16) and patients with other infections (n = 144; all publicly available data). We applied inferential statistics (the COVID-engine platform) to RNA profiles (from limited number of samples) derived from peripheral blood mononuclear cells (PBMCs). Compared to healthy individuals, a subset of integrated blood-based gene profiles (signatures) distinguished acute-like (mimicking coronavirus-infected patients with prolonged hospitalization) from recovering-like patients. These signatures also hierarchically represented multiple (at the system level) parameters associated with PBMC including dysregulated cytokines, genes, pathways, networks of pathways/concepts, immune status, and cell types. Proof-of-principle observations included PBMC-based increases in cytokine storm-associated IL6, enhanced innate immunity (macrophages and neutrophils), and lower adaptive T and B cell immunity in patients with acute-like disease compared to those with recovery-like disease. Patients in the recovery-like stage showed significantly enhanced TNF, IFN-γ, anti-viral, HLA-DQA1, and HLA-F gene expression and cytolytic activity, and reduced pro-viral gene expression compared to those in the acute-like stage in PBMC. Besides, our analysis revealed overlapping genes associated with potential comorbidities (associated diabetes) and disease-like conditions (associated with thromboembolism, pneumonia, lung disease, and septicemia). Overall, our COVID-engine inferential statistics platform and study involving PBMC-based RNA profiling may help understand complex and variable system-wide responses displayed by coronavirus-infected patients with further validation.

Published

2020

14. Harnessing tRNA for Processing Ability and Promoter Activity

Author

David J.H.F. Knapp and Tudor A. Fulga

Subjects

Cloning, 0303 health sciences, Cas9, RNA polymerase II, Computational biology, Biology, Genome engineering, 03 medical and health sciences, 0302 clinical medicine, Genome editing, Transfer RNA, biology.protein, CRISPR, Guide RNA, 030217 neurology & neurosurgery, 030304 developmental biology

Abstract

Transfer RNA (tRNA) and their associated production and processing machinery can be coopted as a versatile tool for the production of guide RNAs (gRNAs) for Cas9-based genome engineering. Using different tRNA variants enables the production of gRNAs at a variety of steady state levels. Furthermore, engineered tRNAs can be used to process gRNAs from Pol-II transcripts, thus enabling spatial/temporal control of gRNA expression. Here we describe the design, cloning, and testing of tRNA scaffolds for both Pol-III-driven expression of different levels of gRNAs, and for processing gRNAs from Pol-II transcripts.

Published

2020

15. A blood-based comprehensive and systems-level analysis of disease stages, immune regulation and symptoms in COVID-19 patients

Author

Tobias Bopp, Nagarajan Kannan, Krishnaraj Rajalingam, Chitra Priya Emperumal, Santosh Dixit, David J.H.F. Knapp, Anguraj Sadanandam, and Alan Melcher

Subjects

Coronavirus disease 2019 (COVID-19), business.industry, Disease stages, Immunology, Immune regulation, Medicine, business

Abstract

COVID-19 patients show significant clinical heterogeneity in presentation and outcomes that makes pandemic control and strategy difficult; optimising management requires a systems biology approach of understanding the disease. Here we sought to understand and infer complex system-wide changes in patients infected with coronaviruses (SARS-CoV and SARS-CoV-2; n=38 and 57 samples) at two different disease stages compared with healthy individuals (n=16) and patients with other infections (n=144). We applied inferential statistics/machine-learning approaches (the COVID-engine platform) to RNA profiles derived from peripheral blood mononuclear cells (PBMCs). Compared to healthy individuals, an integrated blood-based gene signatures distinguished acute-like (mimicking coronavirus-infected patients with prolonged hospitalisation) from recovering-like patients. These signatures also hierarchically represented systems-level parameters associated with PBMC including dysregulated cytokines, genes, pathways, networks of pathways/concepts, immune status, and cell types. Proof-of-principle confirmatory observations included PBMC-associated increases in ACE2, cytokine storm-associated IL6, enhanced innate immunity (macrophages and neutrophils), and lower adaptive T and B cell immunity in patients with acute-like disease compared to those with recovery-like disease. Patients in the recovery-like stage had significantly enhanced TNF, IFN-g, anti-viral, HLA-DQA1, and HLA-F gene expression and cytolytic activity, and reduced pro-viral gene expression compared to those in the acute-like stage in PBMC. Besides, PBMC-derived surrogate-based approach revealed overlapping genes associated with comorbidities (associated diabetes), and disease-like symptoms (associated with thromboembolism, pneumonia, lung disease and septicaemia). Overall, our study involving PBMC-based RNA profiling may further help understand complex and variable systems-wide responses displayed by coronavirus-infected patients.

Published

2020

16. Single-cell analysis identifies a CD33+ subset of human cord blood cells with high regenerative potential

Author

Michelle Moksa, Paul H. Miller, Martin Hirst, Fangwu Wang, Philip A. Beer, Tony Hui, R. Keith Humphries, Connie J. Eaves, Colin A. Hammond, Davide Pellacani, Nima Aghaeepour, Carl L. Hansen, Gabrielle Rabu, Marijn T J van Loenhout, and David J.H.F. Knapp

Subjects

0301 basic medicine, medicine.diagnostic_test, Cell growth, Cell, Cell Biology, Cord Blood Stem Cell Transplantation, Biology, Cell biology, Flow cytometry, 03 medical and health sciences, 030104 developmental biology, medicine.anatomical_structure, Single-cell analysis, Cord blood, DNA methylation, medicine, Mitosis

Abstract

Elucidation of the identity and diversity of mechanisms that sustain long-term human blood cell production remains an important challenge. Previous studies indicate that, in adult mice, this property is vested in cells identified uniquely by their ability to clonally regenerate detectable, albeit highly variable levels and types, of mature blood cells in serially transplanted recipients. From a multi-parameter analysis of the molecular features of very primitive human cord blood cells that display long-term cell outputs in vitro and in immunodeficient mice, we identified a prospectively separable CD33+CD34+CD38-CD45RA-CD90+CD49f+ phenotype with serially transplantable, but diverse, cell output profiles. Single-cell measurements of the mitogenic response, and the transcriptional, DNA methylation and 40-protein content of this and closely related phenotypes revealed subtle but consistent differences both within and between each subset. These results suggest that multiple regulatory mechanisms combine to maintain different cell output activities of human blood cell precursors with high regenerative potential.

Published

2018

17. Mass Cytometric Analysis Reveals Viable Activated Caspase-3+ Luminal Progenitors in the Normal Adult Human Mammary Gland

Author

Davide Pellacani, Connie J. Eaves, Nagarajan Kannan, and David J.H.F. Knapp

Subjects

0301 basic medicine, Cell type, Mammary gland, Caspase 3, Biology, General Biochemistry, Genetics and Molecular Biology, Cell biology, 03 medical and health sciences, 030104 developmental biology, medicine.anatomical_structure, lcsh:Biology (General), Epidermal growth factor, Immunology, medicine, Immunohistochemistry, Mass cytometry, Progenitor cell, Clonogenic assay, lcsh:QH301-705.5

Abstract

Summary: The normal adult human female mammary gland is a bilayered structure consisting of an outer basal layer and two readily distinguished subsets of cells within the inner luminal layer. We now present a validated methodology for undertaking large-scale multi-parameter mass cytometric analyses of these cell types at single-cell resolution. In addition, we show how combining this approach with in vitro clonogenic assays of the proliferative and signaling responses of normal human mammary cells to epidermal growth factor (EGF) allows additional subsets with different EGF responses to be discerned. This included the identification of a subset of cells within the phenotypically defined luminal progenitor fraction that displays an elevated content of active caspase-3, including some that generate clones in vitro in response to EGF, with immunohistochemical evidence of their presence in situ in fixed preparations of normal human breast tissue. : Knapp et al. identify a subpopulation of progenitors in the human mammary gland that have partially activated an apoptotic program despite retaining some viability and clonogenic potential. As such activation has been linked to genomic instability, these cells may be at increased risk for oncogenic transformation. Keywords: mammary, mass cytometry, cancer, apoptosis, signaling, cell death, genomic instability, single-cell biology, growth factors

Published

2017

18. Analysis of parameters that affect human hematopoietic cell outputs in mutant c-kit-immunodeficient mice

Author

Margarita MacAldaz, Connie J. Eaves, Gabrielle Rabu, Naoto Nakamichi, Leonard D. Shultz, Kiran Dhillon, Paul H. Miller, R. Keith Humphries, Philip A. Beer, Alice M.S. Cheung, and David J.H.F. Knapp

Subjects

Male, 0301 basic medicine, Cancer Research, medicine.medical_treatment, Transplantation, Heterologous, CD34, Cell Count, Mice, SCID, Hematopoietic stem cell transplantation, Transplantation Chimera, Nod, Biology, Article, Immunophenotyping, Mice, 03 medical and health sciences, Sex Factors, Mice, Inbred NOD, Genetics, medicine, Animals, Humans, Molecular Biology, Mice, Knockout, Graft Survival, Age Factors, Hematopoietic Stem Cell Transplantation, Cell Biology, Hematology, Hematopoietic Stem Cells, Transplantation, Proto-Oncogene Proteins c-kit, Haematopoiesis, 030104 developmental biology, Cord blood, Mutation, Immunology, Female, Biomarkers

Abstract

Xenograft models are transforming our understanding of the output capabilities of primitive human hematopoietic cells in vivo . However, many variables that affect posttransplantation reconstitution dynamics remain poorly understood. Here, we show that an equivalent level of human chimerism can be regenerated from human CD34 + cord blood cells transplanted intravenously either with or without additional radiation-inactivated cells into 2- to 6-month-old NOD-Rag1 –/– -IL2Rγc –/– (NRG) mice given a more radioprotective conditioning regimen than is possible in conventionally used, repair-deficient NOD- Prkdc scid/scid - IL2Rγc –/– (NSG) hosts. Comparison of sublethally irradiated and non-irradiated NRG mice and W 41 /W 41 derivatives showed superior chimerism in the W 41 -deficient recipients, with some differential effects on different lineage outputs. Consistently superior outputs were observed in female recipients regardless of their genotype, age, or pretransplantation conditioning, with greater differences apparent later after transplantation. These results define key parameters for optimizing the sensitivity and minimizing the intraexperimental variability of human hematopoietic xenografts generated in increasingly supportive immunodeficient host mice.

Published

2017

19. Replication timing alterations in leukemia affect clinically relevant chromosome domains

Author

Juan Carlos Rivera-Mulia, David M. Gilbert, Naoto Nakamichi, Amnon Koren, Tanja A. Gruber, Brian J. Druker, David J.H.F. Knapp, Connie J. Eaves, Kyle N. Klein, Jared P. Zimmerman, Takayo Sasaki, Claudia Trevilla-Garcia, Jeffrey W. Tyner, Vivek Somasundaram, Colin A. Hammond, Bill H. Chang, and Meenakshi Devidas

Subjects

0301 basic medicine, Male, Cell type, Hematopoiesis and Stem Cells, DNA Replication Timing, CD34, Biology, Chromosomes, Immunophenotyping, Central Nervous System Neoplasms, 03 medical and health sciences, Mice, 0302 clinical medicine, Precursor B-Cell Lymphoblastic Leukemia-Lymphoma, medicine, Animals, Humans, Epigenetics, Mice, Knockout, Replication timing, B-Lymphocytes, Leukemia, Gene Expression Profiling, Chromosome, Computational Biology, Genetic Variation, Hematology, medicine.disease, Hematopoietic Stem Cells, Disease Models, Animal, 030104 developmental biology, 030220 oncology & carcinogenesis, Cord blood, Cancer research, Disease Progression, Heterografts, Female, Disease Susceptibility, Biomarkers

Abstract

Human B-cell precursor acute lymphoid leukemias (BCP-ALLs) comprise a group of genetically and clinically distinct disease entities with features of differentiation arrest at known stages of normal B-lineage differentiation. We previously showed that BCP-ALL cells display unique and clonally heritable, stable DNA replication timing (RT) programs (ie, programs describing the variable order of replication and subnuclear 3D architecture of megabase-scale chromosomal units of DNA in different cell types). To determine the extent to which BCP-ALL RT programs mirror or deviate from specific stages of normal human B-cell differentiation, we transplanted immunodeficient mice with quiescent normal human CD34+ cord blood cells and obtained RT signatures of the regenerating B-lineage populations. We then compared these with RT signatures for leukemic cells from a large cohort of BCP-ALL patients with varied genetic subtypes and outcomes. The results identify BCP-ALL subtype-specific features that resemble specific stages of B-cell differentiation and features that seem to be associated with relapse. These results suggest that the genesis of BCP-ALL involves alterations in RT that reflect biologically significant and potentially clinically relevant leukemia-specific epigenetic changes.

Published

2019

20. Polycomb contraction differentially regulates terminal human hematopoietic differentiation programs

Author

Martin Hirst, Jasper Wong, Alireza Heravi-Moussavi, Michelle Moksa, Marcus Wong, Annaick Carles, Connie J. Eaves, David J.H.F. Knapp, Colin A. Hammond, Alireza Lorzadeh, Qi Cao, Misha Bilenky, Sharafian Z, Zhu J, Pascal M. Lavoie, and F. Wang

Subjects

0303 health sciences, Myeloid, Contraction (grammar), Monocyte, macromolecular substances, Biology, Phenotype, Cell biology, 03 medical and health sciences, Haematopoiesis, 0302 clinical medicine, medicine.anatomical_structure, medicine, Epigenetics, Progenitor cell, Transcription factor, 030217 neurology & neurosurgery, 030304 developmental biology

Abstract

Lifelong production of the many types of mature blood cells from less differentiated progenitors is a hierarchically ordered process that spans multiple cell divisions. The nature and timing of the molecular events required to integrate the environmental signals, transcription factor activity, epigenetic modifications, and changes in gene expression involved are thus complex and still poorly understood. We now show that the more primitive types of human cells in this system display a unique repressive H3K27me3 signature that is retained by mature lymphoid cells but is lost in terminally differentiated monocytes and erythroblasts. Additional intervention data implicate that control of this chromatin state change is a requisite part of the process, whereby normal human hematopoietic progenitor cells make lymphoid and myeloid fate decisions.

Published

2019

21. Variable Retention of Differentiation-specific DNA Replication Timing in Human Pediatric Leukemia

Author

David M. Gilbert, Jared P. Zimmerman, Tanja A. Gruber, Meenakshi Devidas, Vivek Somasundaram, Amnon Koren, Kyle N. Klein, David J.H.F. Knapp, Naoto Nakamichi, Brian J. Druker, Connie J. Eaves, Juan Carlos Rivera-Mulia, Colin A. Hammond, Bill H. Chang, Claudia Trevilla-Garcia, Takayo Sasaki, and Jeffrey W. Tyner

Subjects

0303 health sciences, Replication timing, Cell type, CD34, Biology, medicine.disease, Genome, 03 medical and health sciences, Leukemia, 0302 clinical medicine, 030220 oncology & carcinogenesis, Cord blood, DNA Replication Timing, Cancer research, medicine, Epigenetics, 030304 developmental biology

Abstract

Human B-lineage precursor acute lymphoid leukemias (BCP-ALLs) comprise a group of genetically and clinically distinct disease entities with features of differentiation arrest at known stages of normal B-lineage differentiation. We previously showed BCP-ALL cells display unique and clonally heritable DNA-replication timing (RT) programs; i.e., programs describing the variable order of replication of megabase-scale chromosomal units of DNA in different cell types. To determine the extent to which BCP-ALL RT programs mirror or deviate from specific stages of normal human B-cell differentiation, we transplanted immunodeficient mice with quiescent normal human CD34+ cord blood cells and obtained RT signatures of the regenerating B-lineage populations. We then compared these with RT signatures for leukemic cells from a large cohort of BCP-ALL patients. The results identify BCP-ALL subtype-specific features that resemble specific stages of B-cell differentiation and features that appear associated with relapse. These results suggest the genesis of BCP-ALL involves alterations in RT that reflect clinically relevant leukemia-specific genetic and/or epigenetic changes.SUMMARYGenome-wide DNA replication timing profiles of >100 pediatric leukemic samples and normally differentiating human B-lineage cells isolated from xenografted immunodeficient mice were generated. Comparison of these identified potentially clinically relevant features that both match and deviate from the normal profiles.

Published

2019

22. GateFinder: projection-based gating strategy optimization for flow and mass cytometry

Author

Sean C. Bendall, Connie J. Eaves, Robert V. Bruggner, Gabriela K. Fragiadakis, Nikolay Samusik, Pier Federico Gherardini, Karen Sachs, Erin F. Simonds, William A. Weiss, Garry P. Nolan, Brice Gaudilliere, Martin S. Angst, Anthony Culos, David J.H.F. Knapp, Nima Aghaeepour, Wendy J. Fantl, and Wren, Jonathan

Subjects

0301 basic medicine, Statistics and Probability, Bioinformatics, Gating, computer.software_genre, Biochemistry, Mathematical Sciences, Bioconductor, 03 medical and health sciences, 0302 clinical medicine, Information and Computing Sciences, medicine, Mass cytometry, Projection (set theory), Molecular Biology, Supplementary data, Settore BIO/11, Biological Sciences, Complex cell, Flow Cytometry, Applications Notes, Computer Science Applications, Computational Mathematics, 030104 developmental biology, medicine.anatomical_structure, Computational Theory and Mathematics, Flow (mathematics), 030220 oncology & carcinogenesis, Polygon, Data mining, computer, Algorithms, Biomarkers, Software

Abstract

Motivation High-parameter single-cell technologies can reveal novel cell populations of interest, but studying or validating these populations using lower-parameter methods remains challenging. Results Here, we present GateFinder, an algorithm that enriches high-dimensional cell types with simple, stepwise polygon gates requiring only two markers at a time. A series of case studies of complex cell types illustrates how simplified enrichment strategies can enable more efficient assays, reveal novel biomarkers and clarify underlying biology. Availability and implementation The GateFinder algorithm is implemented as a free and open-source package for BioConductor: https://nalab.stanford.edu/gatefinder. Supplementary information Supplementary data are available at Bioinformatics online.

Published

2018

23. Analysis of Normal Human Mammary Epigenomes Reveals Cell-Specific Active Enhancer States and Associated Transcription Factor Networks

Author

Marco A. Marra, Steven J.M. Jones, Samuel Aparicio, Nagarajan Kannan, Martin Hirst, Michelle Moksa, Annaick Carles, Alireza Heravi-Moussavi, David J.H.F. Knapp, Davide Pellacani, Richard A. Moore, Sitanshu Gakkhar, Andrew J. Mungall, Misha Bilenky, and Connie J. Eaves

Subjects

Adult, 0301 basic medicine, Cell type, Cell Separation, Biology, epigenomic, General Biochemistry, Genetics and Molecular Biology, Epigenesis, Genetic, regulatory network, 03 medical and health sciences, stem cells, transcription factors, Humans, Gene Regulatory Networks, normal human breast, Breast, Progenitor cell, Promoter Regions, Genetic, Enhancer, Transcription factor, Epigenomics, Myoepithelial cell, Reproducibility of Results, Epithelial Cells, Molecular biology, Chromatin, Enhancer Elements, Genetic, Phenotype, 030104 developmental biology, Regulatory sequence, chromatin, Female, enhancer, profiling, mammary cells, transcriptome

Abstract

SummaryThe normal adult human mammary gland is a continuous bilayered epithelial system. Bipotent and myoepithelial progenitors are prominent and unique components of the outer (basal) layer. The inner (luminal) layer includes both luminal-restricted progenitors and a phenotypically separable fraction that lacks progenitor activity. We now report an epigenomic comparison of these three subsets with one another, with their associated stromal cells, and with three immortalized, non-tumorigenic human mammary cell lines. Each genome-wide analysis contains profiles for six histone marks, methylated DNA, and RNA transcripts. Analysis of these datasets shows that each cell type has unique features, primarily within genomic regulatory regions, and that the cell lines group together. Analyses of the promoter and enhancer profiles place the luminal progenitors in between the basal cells and the non-progenitor luminal subset. Integrative analysis reveals networks of subset-specific transcription factors.

Published

2016

24. Nucleosome Density ChIP-Seq Identifies Distinct Chromatin Modification Signatures Associated with MNase Accessibility

Author

Alireza Lorzadeh, Sitanshu Gakkhar, Misha Bilenky, Martin Hirst, Michelle Moksa, Paul H. Miller, Luolan Li, Colin A. Hammond, Annaick Carles, David J.H.F. Knapp, Alireza Heravi-Moussavi, and Connie J. Eaves

Subjects

0301 basic medicine, Chromatin Immunoprecipitation, Human Embryonic Stem Cells, Antigens, CD34, Biology, bivalent promoter, General Biochemistry, Genetics and Molecular Biology, Histones, 03 medical and health sciences, Histone H1, cellular heterogeneity, Histone H2A, Histone methylation, Humans, Histone code, Nucleosome, histone modification, Histone octamer, nucleosome density, Promoter Regions, Genetic, Genetics, Sequence Analysis, RNA, Gene Expression Profiling, DNA, DNA Methylation, Fetal Blood, Linker DNA, Nucleosomes, Cell biology, ChIP-seq, 030104 developmental biology, Gene Expression Regulation, Histone methyltransferase, epigenomics, RNA, micrococcal nuclease, CpG Islands, Protein Processing, Post-Translational

Abstract

SummaryNucleosome position, density, and post-translational modification are widely accepted components of mechanisms regulating DNA transcription but still incompletely understood. We present a modified native ChIP-seq method combined with an analytical framework that allows MNase accessibility to be integrated with histone modification profiles. Application of this methodology to the primitive (CD34+) subset of normal human cord blood cells enabled genomic regions enriched in one versus two nucleosomes marked by histone 3 lysine 4 trimethylation (H3K4me3) and/or histone 3 lysine 27 trimethylation (H3K27me3) to be associated with their transcriptional and DNA methylation states. From this analysis, we defined four classes of promoter-specific profiles and demonstrated that a majority of bivalent marked promoters are heterogeneously marked at a single-cell level in this primitive cell type. Interestingly, extension of this approach to human embryonic stem cells revealed an altered relationship between chromatin modification state and nucleosome content at promoters, suggesting developmental stage-specific organization of histone methylation states.

Published

2016

25. Quantitation of Human Cells that Produce Neutrophils and Platelets in Vivo Obtained from Normal Donors Treated with Granulocyte Colony–Stimulating Factor and/or Plerixafor

Author

Stephen Couban, Connie J. Eaves, Kirk R. Schultz, Naoto Nakamichi, David Jones, Paul H. Miller, Gabrielle Rabu, and David J.H.F. Knapp

Subjects

Blood Platelets, 0301 basic medicine, Benzylamines, Myeloid, Neutrophils, Cell Culture Techniques, CD34, Antigens, CD34, Cell Count, Mice, SCID, Granulocyte, Cyclams, Mice, 03 medical and health sciences, 0302 clinical medicine, Heterocyclic Compounds, In vivo, Granulocyte Colony-Stimulating Factor, Animals, Humans, Medicine, Transplantation, business.industry, Plerixafor, Hematology, Hematopoietic Stem Cell Mobilization, In vitro, 3. Good health, Granulocyte colony-stimulating factor, Haematopoiesis, 030104 developmental biology, medicine.anatomical_structure, Immunology, Heterografts, business, 030215 immunology, medicine.drug

Abstract

Plerixafor (P) together with granulocyte colony–stimulating factor (G) is now recognized as an important strategy for mobilizing hematopoietic cells for use in patients given myelosuppressive therapies. However, quantitative comparisons of their ability to mobilize human cells with different hematopoietic activities in vitro or in vivo (in immunodeficient mice) and their interrelationships have not been investigated. To address these questions, we collected samples from 5 normal adult volunteers before and after administering P alone and from another 5 before and after a 4-day course of G and again after a subsequent injection of P. Measurements of their blood content of CD34+ cells, in vitro myeloid colony–forming cells, 3- and 6-week long-term culture (LTC) cell outputs, and levels of circulating human platelets, as well as myeloid and lymphoid cells obtained in immunodeficient mice that received transplants, showed all activities were maximal 4 hours after P preceded by G, and 3-week LTC outputs showed the highest concordance with the 3-week circulating human neutrophil levels obtained in mice that received transplants. Thus, human cells capable of producing neutrophils rapidly in vivo were optimally mobilized by the G + P protocol, and the 3-week LTC assay appears to offer a more specific predictor of their levels than conventional CD34+ cell or colony-forming cell counts.

Published

2016

26. Hematopoietic Stem Cells Are the Major Source of Multilineage Hematopoiesis in Adult Animals

Author

Samik Upadhaya, Connie J. Eaves, Sonja Babovic, Joji Fujisaki, Boris Reizis, Leonid A. Mirny, Jue Feng, Lei Ding, Yonit Lavin, David J.H.F. Knapp, Miriam Merad, Anton Goloborodko, Catherine M. Sawai, Colleen M. Lau, Institute for Medical Engineering and Science, Massachusetts Institute of Technology. Department of Physics, Goloborodko, Anton, and Mirny, Leonid A

Subjects

0301 basic medicine, medicine.medical_treatment, Transgene, Immunology, hemic and immune systems, Biology, Cell biology, Transplantation, 03 medical and health sciences, Haematopoiesis, 030104 developmental biology, 0302 clinical medicine, Infectious Diseases, Immune system, Cytokine, Interferon, 030220 oncology & carcinogenesis, medicine, Immunology and Allergy, Progenitor cell, Stem cell, medicine.drug

Abstract

Hematopoietic stem cells (HSCs) sustain long-term reconstitution of hematopoiesis in transplantation recipients, yet their role in the endogenous steady-state hematopoiesis remains unclear. In particular, recent studies suggested that HSCs provide a relatively minor contribution to immune cell development in adults. We directed transgene expression in a fraction of HSCs that maintained reconstituting activity during serial transplantations. Inducible genetic labeling showed that transgene-expressing HSCs gave rise to other phenotypic HSCs, confirming their top position in the differentiation hierarchy. The labeled HSCs rapidly contributed to committed progenitors of all lineages and to mature myeloid cells and lymphocytes, but not to B-1a cells or tissue macrophages. Importantly, labeled HSCs gave rise to more than two-thirds of all myeloid cells and platelets in adult mice, and this contribution could be accelerated by an induced interferon response. Thus, classically defined HSCs maintain immune cell development in the steady state and during systemic cytokine responses.

Published

2016

27. High-Resolution Single-Cell DNA Methylation Measurements Reveal Epigenetically Distinct Hematopoietic Stem Cell Subpopulations

Author

Samuel Aparicio, Emma Laks, Qi Cao, Aly Karsan, Colin A. Hammond, Joanna Wegrzyn-Woltosz, Michelle Moksa, Martin Hirst, Connie J. Eaves, David J.H.F. Knapp, Kieran O'Neill, and Tony Hui

Subjects

0301 basic medicine, Resource, Bisulfite sequencing, Computational biology, Biology, Biochemistry, Epigenesis, Genetic, 03 medical and health sciences, Mice, Single-cell analysis, Genetics, medicine, Animals, Epigenetics, lcsh:QH301-705.5, lcsh:R5-920, DNA methylation, epigenetics, Gene Expression Profiling, Hematopoietic stem cell, Computational Biology, Cell Biology, Methylation, Genomics, Hematopoietic Stem Cells, 3. Good health, single cell, 030104 developmental biology, medicine.anatomical_structure, CpG site, lcsh:Biology (General), CpG Islands, hematopoietic stem cell, Stem cell, Single-Cell Analysis, lcsh:Medicine (General), Developmental Biology

Abstract

Summary Increasing evidence of functional and transcriptional heterogeneity in phenotypically similar cells examined individually has prompted interest in obtaining parallel methylome data. We describe the development and application of such a protocol to index-sorted murine and human hematopoietic cells that are highly enriched in their content of functionally defined stem cells. Utilizing an optimized single-cell bisulfite sequencing protocol, we obtained quantitative DNA methylation measurements of up to 5.7 million CpGs in single hematopoietic cells. In parallel, we developed an analytical strategy (PDclust) to define single-cell DNA methylation states through pairwise comparisons of single-CpG methylation measurements. PDclust revealed that a single-cell epigenetic state can be described by a small (, Highlights • DNA methylation measurements of up to 5.7 million CpGs in a single cell • Methylation signatures within hematopoietic stem cells are highly redundant • Stem cell populations contain rare epigenetically distinct subpopulations • Comprehensive single-cell CpG measurements allow for regulatory state annotation, We present a single-cell methylation protocol and novel analytical method to enable high-resolution reconstruction of regulatory states within rare epigenetically distinct subpopulations of highly purified murine and human hematopoietic stem cells. Pairwise single-CpG-based analysis revealed a high degree of redundancy in single-cell epigenetic states.

Published

2018

28. Disruption of IKAROS activity in primitive chronic-phase CML cells mimics myeloid disease progression

Author

Gabrielle Rabu, Brian J. Druker, Jefferson Terry, Nagarajan Kannan, Jerald P. Radich, Philip A. Beer, Ivan Sloma, Sonja Babovic, Elizabeth Bulaeva, Wendy N. Erber, Keith R. Loeb, Marc M. Loriaux, David J.H.F. Knapp, Paul H. Miller, Connie J. Eaves, and Kathy Heel

Subjects

Myeloid, Cellular differentiation, Blotting, Western, Immunology, CD34, Antigens, CD34, Apoptosis, Mice, SCID, Biology, Real-Time Polymerase Chain Reaction, Biochemistry, Immunoenzyme Techniques, Ikaros Transcription Factor, Mice, Mice, Inbred NOD, hemic and lymphatic diseases, STAT5 Transcription Factor, medicine, Animals, Humans, RNA, Messenger, neoplasms, Protein Kinase Inhibitors, Cells, Cultured, Cell Proliferation, Acute leukemia, Myeloid Neoplasia, Reverse Transcriptase Polymerase Chain Reaction, Myeloid leukemia, Cell Differentiation, Cell Biology, Hematology, Protein-Tyrosine Kinases, Flow Cytometry, medicine.disease, Basophils, Eosinophils, Leukemia, medicine.anatomical_structure, Leukemia, Myeloid, Chronic-Phase, Disease Progression, Cancer research, Bone marrow

Abstract

Without effective therapy, chronic-phase chronic myeloid leukemia (CP-CML) evolves into an acute leukemia (blast crisis [BC]) that displays either myeloid or B-lymphoid characteristics. This transition is often preceded by a clinically recognized, but biologically poorly characterized, accelerated phase (AP). Here, we report that IKAROS protein is absent or reduced in bone marrow blasts from most CML patients with advanced myeloid disease (AP or BC). This contrasts with primitive CP-CML cells and BCR-ABL1-negative acute myeloid leukemia blasts, which express readily detectable IKAROS. To investigate whether loss of IKAROS contributes to myeloid disease progression in CP-CML, we examined the effects of forced expression of a dominant-negative isoform of IKAROS (IK6) in CP-CML patients' CD34(+) cells. We confirmed that IK6 disrupts IKAROS activity in transduced CP-CML cells and showed that it confers on them features of AP-CML, including a prolonged increased output in vitro and in xenografted mice of primitive cells with an enhanced ability to differentiate into basophils. Expression of IK6 in CD34(+) CP-CML cells also led to activation of signal transducer and activator of transcription 5 and transcriptional repression of its negative regulators. These findings implicate loss of IKAROS as a frequent step and potential diagnostic harbinger of progressive myeloid disease in CML patients.

Published

2015

29. A Dominant-Negative Isoform of IKAROS Expands Primitive Normal Human Hematopoietic Cells

Author

Nima Aghaeepour, Gabrielle Rabu, Lisa Wei, Connie J. Eaves, Sonja Babovic, Philip A. Beer, Elizabeth Bulaeva, Shabnam Rostamirad, David J.H.F. Knapp, Paul H. Miller, Nagarajan Kannan, and Kingsley Shih

Subjects

medicine.medical_treatment, Cellular differentiation, Mice, SCID, Hematopoietic stem cell transplantation, Biochemistry, 0302 clinical medicine, Mice, Inbred NOD, Protein Isoforms, lcsh:QH301-705.5, Cells, Cultured, Mice, Knockout, lcsh:R5-920, B-Lymphocytes, 0303 health sciences, Microscopy, Confocal, Hematopoietic Stem Cell Transplantation, Cell Differentiation, Fetal Blood, Ikaros Transcription Factor, Cell biology, Haematopoiesis, Leukemia, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Cord blood, lcsh:Medicine (General), Interleukin Receptor Common gamma Subunit, Blotting, Western, Transplantation, Heterologous, Biology, Article, 03 medical and health sciences, Genetics, medicine, Animals, Humans, B cell, Cell Proliferation, 030304 developmental biology, Cell growth, Gene Expression Profiling, Cell Biology, Hematopoietic Stem Cells, medicine.disease, Molecular biology, Mice, Inbred C57BL, lcsh:Biology (General), Granulocytes, HeLa Cells, Developmental Biology

Abstract

Summary Disrupted IKAROS activity is a recurrent feature of some human leukemias, but effects on normal human hematopoietic cells are largely unknown. Here, we used lentivirally mediated expression of a dominant-negative isoform of IKAROS (IK6) to block normal IKAROS activity in primitive human cord blood cells and their progeny. This produced a marked (10-fold) increase in serially transplantable multipotent IK6+ cells as well as increased outputs of normally differentiating B cells and granulocytes in transplanted immunodeficient mice, without producing leukemia. Accompanying T/natural killer (NK) cell outputs were unaltered, and erythroid and platelet production was reduced. Mechanistically, IK6 specifically increased human granulopoietic progenitor sensitivity to two growth factors and activated CREB and its targets (c-FOS and Cyclin B1). In more primitive human cells, IK6 prematurely initiated a B cell transcriptional program without affecting the hematopoietic stem cell-associated gene expression profile. Some of these effects were species specific, thus identifying novel roles of IKAROS in regulating normal human hematopoietic cells., Graphical Abstract, Highlights • IKAROS protein is abundantly expressed in primitive human hematopoietic cells • IK6 enhances human blood stem cell expansion in vivo without causing leukemia • IK6 has a unique profile of lineage-specific effects on human hematopoietic cells • IK6 activates B-lineage transcripts prematurely in human blood stem cells, This study reveals a role for IKAROS in the regulation of normal human hematopoietic stem cells (HSCs). In this report, Eaves and colleagues demonstrate that disruption of IKAROS activity expands human HSCs and enhances their outputs of normally differentiating granulocytic and B-lineage cells, without inducing leukemic transformation.

Published

2014

30. Pyrimidoindole derivatives are agonists of human hematopoietic stem cell self-renewal

Author

Sandra Cohen, R. Keith Humphries, Mor Ngom, Stéphane Gingras, Anne Marinier, Denis-Claude Roy, Suzan Imren, Connie J. Eaves, Elizabeth Csaszar, Réjean Ruel, Norman N. Iscove, Guy Sauvageau, Yves Gareau, David J.H.F. Knapp, Nadine Mayotte, Peter W. Zandstra, Hans-Peter Kiem, Robert Herrington, Jalila Chagraoui, Korashon L. Watts, Iman Fares, and Paul H. Miller

Subjects

Indoles, medicine.medical_treatment, Cell Culture Techniques, Stem cell factor, Hematopoietic stem cell transplantation, Biology, CXCR4, Article, Small Molecule Libraries, Immunocompromised Host, Mice, medicine, Animals, Humans, Regeneration, Progenitor cell, Multidisciplinary, Hematopoietic Stem Cell Transplantation, Hematopoietic stem cell, Genetic Therapy, Fetal Blood, Hematopoietic Stem Cells, Hematopoiesis, Endothelial stem cell, Haematopoiesis, Pyrimidines, medicine.anatomical_structure, Receptors, Aryl Hydrocarbon, Cord blood, Immunology, Cancer research

Abstract

Human adult stem cell expansion Transfused blood saves lives. Despite the widespread use of this critical resource, it is difficult to increase blood cell numbers outside of the body. By screening thousands of small compounds, Fares et al. identify a molecule that expands human stem cell numbers in cord blood. The researchers generate many variations of that molecule and show that one such compound provides even greater human blood cell expansion. If researchers can provide increased numbers of stem cells and progenitor cells, cord blood should find even greater use in the clinic. Science , this issue p. 1509

Published

2014

31. Distinct Stromal Cell Factor Combinations Can Separately Control Hematopoietic Stem Cell Survival, Proliferation, and Self-Renewal

Author

David G. Kent, Keegan Rowe, Claudia Benz, Connie J. Eaves, David J.H.F. Knapp, Michael R. Copley, Stefan Wöhrer, Robert A.J. Oostendorp, Heidi Mader, and Sonja Babovic

Subjects

Stromal cell, Cell Survival, Cellular differentiation, Stem cell factor, Biology, Article, General Biochemistry, Genetics and Molecular Biology, Blood cell, Mice, medicine, Animals, Humans, lcsh:QH301-705.5, Cells, Cultured, Cell Proliferation, Cell growth, Hematopoietic stem cell, Cell Differentiation, hemic and immune systems, Hematopoietic Stem Cells, Cell biology, Mice, Inbred C57BL, Haematopoiesis, medicine.anatomical_structure, lcsh:Biology (General), Stromal Cells, Stem cell

Abstract

Summary Hematopoietic stem cells (HSCs) are identified by their ability to sustain prolonged blood cell production in vivo, although recent evidence suggests that durable self-renewal (DSR) is shared by HSC subtypes with distinct self-perpetuating differentiation programs. Net expansions of DSR-HSCs occur in vivo, but molecularly defined conditions that support similar responses in vitro are lacking. We hypothesized that this might require a combination of factors that differentially promote HSC viability, proliferation, and self-renewal. We now demonstrate that HSC survival and maintenance of DSR potential are variably supported by different Steel factor (SF)-containing cocktails with similar HSC-mitogenic activities. In addition, stromal cells produce other factors, including nerve growth factor and collagen 1, that can antagonize the apoptosis of initially quiescent adult HSCs and, in combination with SF and interleukin-11, produce >15-fold net expansions of DSR-HSCs ex vivo within 7 days. These findings point to the molecular basis of HSC control and expansion., Graphical Abstract, Highlights • HSC viability, mitogenesis, and self-renewal are differentially controlled • Stromal cells produce nonmitogenic factors that directly sustain HSC viability • More adult bone marrow cells can produce HSCs than display HSC activity directly • Nerve growth factor and collagen 1 promote serially transplantable HSCs, Wohrer et al. now show that different factors secreted by stromal cells separately control the survival, proliferation, and self-renewal of hematopoietic stem cells. These factors are thus required in combination to stimulate net expansions of these cells with full retention of their original stem cell properties.

Published

2014

32. 1032 - PROSPECTIVE ANALYSIS OF THE HUMAN LEUKEMOGENIC PROCESS

Author

David J.H.F. Knapp, Martin Hirst, Andrew P. Weng, Brian T. Wilhelm, Elizabeth Bulaeva, Colin A. Hammond, Philip A. Beer, Alireza Lorzadeh, Davide Pellacani, Connie J. Eaves, Ivan Sloma, and Naoto Nakamichi

Subjects

Cancer Research, Myeloid, ved/biology, Growth factor, medicine.medical_treatment, ved/biology.organism_classification_rank.species, Hematopoietic stem cell, Cell Biology, Hematology, Biology, Leukemogenic, Haematopoiesis, medicine.anatomical_structure, Cord blood, Genetics, medicine, Cancer research, Model organism, Molecular Biology, Gene

Abstract

Acute myeloid leukemias (AML) comprise a genetically diverse group of human hematologic malignancies with a generally poor prognosis and modes of pathogenesis that have been difficult to investigate. Historic evidence and more recent findings have identified hematopoietic stem cell programs as major targets of mutations that predispose to and/or initiate a multistep process of transformation. However, details of the changes involved and how they interact in emerging human leukemic cells have been particularly challenging to characterize. This is due to an emerging appreciation of the heterogeneity in events that impact the differentiation processes of normal human hematopoietic cells, as well as difficulties in recreating the full leukemogenic alterations in the actual human cells affected, to avoid discrepancies inherent in studying model organisms. Here we describe several models of de novo human leukemogenesis that illustrate their power and the novel results they can generate. These include our recent discovery of a novel “latent” leukemic state that can be obtained in MYC-transduced human cord blood cells regenerating a normal spectrum of lymphoid and myeloid progeny in transplanted immunodeficient mice, but that can then be rapidly activated to an aggressive form of AML by in vivo exposure to a single human growth factor. These findings portend the future utility of de novo human leukemogenesis models as new platforms for elucidating shared molecular mechanisms responsible for different stages of human leukemogenesis that may be initiated by different mutations or exposure to different microenvironmental conditions. The flexibility and consistency of these models also make them attractive for identifying and testing new treatment strategies targeting mechanisms required for disease manifestation.

Published

2019

33. Analysis of the clonal growth and differentiation dynamics of primitive barcoded human cord blood cells in NSG mice

Author

Annaick Carles, David J.H.F. Knapp, Philip A. Beer, Alice M.S. Cheung, Connie J. Eaves, Martin Hirst, Paul H. Miller, Long V. Nguyen, and Kiran Dhillon

Subjects

Time Factors, Hematopoiesis and Stem Cells, Cellular differentiation, Green Fluorescent Proteins, Molecular Sequence Data, Transplantation, Heterologous, Immunology, Oligonucleotides, CD34, Antigens, CD34, Mice, SCID, Cord Blood Stem Cell Transplantation, Biology, Biochemistry, Immunophenotyping, Flow cytometry, Mice, Mice, Inbred NOD, medicine, Animals, DNA Barcoding, Taxonomic, Humans, Cell Lineage, Cell Proliferation, Mice, Knockout, Base Sequence, medicine.diagnostic_test, Cell growth, Hematopoietic stem cell, Cell Differentiation, Cell Biology, Hematology, Fetal Blood, Flow Cytometry, Molecular biology, Clone Cells, Kinetics, medicine.anatomical_structure, Cord blood, HeLa Cells, Interleukin Receptor Common gamma Subunit

Abstract

Human cord blood (CB) offers an attractive source of cells for clinical transplants because of its rich content of cells with sustained repopulating ability in spite of an apparent deficiency of cells with rapid reconstituting ability. Nevertheless, the clonal dynamics of nonlimiting CB transplants remain poorly understood. To begin to address this question, we exposed CD34+ CB cells to a library of barcoded lentiviruses and used massively parallel sequencing to quantify the clonal distributions of lymphoid and myeloid cells subsequently detected in sequential marrow aspirates obtained from 2 primary NOD/SCID-IL2Rγ(-/-) mice, each transplanted with ∼10(5) of these cells, and for another 6 months in 2 secondary recipients. Of the 196 clones identified, 68 were detected at 4 weeks posttransplant and were often lympho-myeloid. The rest were detected later, after variable periods up to 13 months posttransplant, but with generally increasing stability throughout time, and they included clones in which different lineages were detected. However, definitive evidence of individual cells capable of generating T-, B-, and myeloid cells, for over a year, and self-renewal of this potential was also obtained. These findings highlight the caveats and utility of this model to analyze human hematopoietic stem cell control in vivo.

Published

2013

34. Heterogeneity in hematopoietic stem cell populations

Author

David J.H.F. Knapp, Paul H. Miller, and Connie J. Eaves

Subjects

Cell type, Hematopoietic Stem Cell Transplantation, Hematopoietic stem cell, Hematology, Biology, Hematopoietic Stem Cells, Cell biology, Transplantation, Blood cell, Haematopoiesis, medicine.anatomical_structure, medicine, Humans, Cell Lineage, Repopulation, Stem cell, Cell Proliferation, Signal Transduction

Abstract

PURPOSE OF REVIEW Transplantation of hematopoietic cells is now a well established clinical procedure, although optimal outcomes are not always obtained. This reflects insufficient knowledge of the different subsets of primitive cells required to achieve a rapid and permanent recovery of mature blood cell production. Here we review recent findings that extend our understanding of these cells and their regulation, and implications for the ex-vivo expansion of these cells. RECENT FINDINGS Separate subsets of platelet and neutrophil lineage-restricted human hematopoietic cells with rapid but transient repopulating activities have been identified, thus adding to previous evidence of short-term repopulating cells that generate both of these lineages. New studies also suggest intrinsically determined heterogeneity in differentiation potentialities that are sustained at the stem cell level, and have revealed new ways their self-renewal can be influenced. SUMMARY Hematopoietic repopulation posttransplant is highly complex both in terms of the differing numbers and types of cells required for optimal hematopoietic recoveries and the factors that will determine the composition and behavior of a given inoculum. Successful ex-vivo expansion protocols will, thus, need to incorporate conditions that will produce adequate numbers of all cell types required with retention of their full functionality.

Published

2013

35. Factors Influencing the Sensitivity and Specificity of Conventional Sequencing in Human Immunodeficiency Virus Type 1 Tropism Testing

Author

Xiaoyin Zhong, Winnie Dong, Rachel A. McGovern, P. R. Harrigan, David J.H.F. Knapp, Art F. Y. Poon, Luke C. Swenson, and Conan K. Woods

Subjects

Microbiology (medical), Genotype, Genotyping Techniques, Population, HIV Infections, Genome, Viral, Biology, V3 loop, Virus Replication, Sensitivity and Specificity, Deep sequencing, chemistry.chemical_compound, Virology, Humans, education, Genetic Association Studies, Tropism, Maraviroc, Genetics, education.field_of_study, Base Sequence, High-Throughput Nucleotide Sequencing, Reproducibility of Results, Replicate, Viral Load, Viral Tropism, Phenotype, chemistry, HIV-1, Tissue tropism, Viral load

Abstract

Human immunodeficiency virus type 1 (HIV-1) V3 loop sequence can be used to infer viral coreceptor use. The effect of input copy number on population-based sequencing of the V3 loop of HIV-1 was examined through replicate deep and population-based sequencing of samples with known tropism, a heterogeneous clinical sample (624 population-based sequences and 47 deep-sequencing replicates), and a large cohort of clinical samples from phase III clinical trials of maraviroc including the MOTIVATE/A4001029 studies ( n = 1,521). Proviral DNA from two independent samples from each of 101 patients from the MOTIVATE/A4001029 studies was also analyzed. Cumulative technical error occurred at a rate of 3 × 10 −4 mismatches/bp, without observed effect on inferred tropism. Increasing PCR replication increased minority species detection with an ∼10% minority population detected in 18% of cases using a single replicate at a viral load of 1,072 copies/ml and in 44% of cases using three replicates. The nucleotide prevalence detected by population-based and deep sequencing were highly correlated (Spearman's ρ, 0.73), and the accuracy increased with increasing input copy number ( P < 0.001). Triplicate sequencing was able to predict tropism changes in the MOTIVATE/A4001029 studies for both low ( P = 0.05) and high ( P = 0.02) viral loads. Sequences derived from independently extracted and processed samples of proviral DNA for the same patient were equivalent to replicates from the same extraction ( P = 0.45) and had correlated position-specific scoring matrix scores (Spearman's ρ, 0.75; P ≪ 0.001); however, concordance in tropism inference was only 83%. Input copy number and PCR replication are important factors in minority species detection in samples with significant heterogeneity.

Published

2013

36. Enhanced normal short-term human myelopoiesis in mice engineered to express human-specific myeloid growth factors

Author

Alice M.S. Cheung, Shabnam Rostamirad, David J.H.F. Knapp, R. Keith Humphries, Gabrielle Rabu, Paul H. Miller, Philip A. Beer, Kiran Dhillon, and Connie J. Eaves

Subjects

Time Factors, Myeloid, Neutrophils, Transplantation, Heterologous, Immunology, Mice, SCID, Nod, Biology, Biochemistry, Mice, Mice, Inbred NOD, medicine, Animals, Humans, Mice, Knockout, Myelopoiesis, Severe combined immunodeficiency, Graft Survival, Granulocyte-Macrophage Colony-Stimulating Factor, Cell Biology, Hematology, medicine.disease, Colony-stimulating factor, Transplantation, Haematopoiesis, medicine.anatomical_structure, Granulocyte macrophage colony-stimulating factor, Cancer research, Interleukin-3, Cord Blood Stem Cell Transplantation, medicine.drug

Abstract

Better methods to characterize normal human hematopoietic cells with short-term repopulating activity cells (STRCs) are needed to facilitate improving recovery rates in transplanted patients.We now show that 5-fold more human myeloid cells are produced in sublethally irradiated NOD/SCID-IL-2Receptor-γchain-null (NSG) mice engineered to constitutively produce human interleukin-3, granulocyte-macrophage colony-stimulating factor and Steel factor (NSG-3GS mice) than in regular NSG mice 3 weeks after an intravenous injection of CD34 human cord blood cells. Importantly, the NSG-3GS mice also show a concomitant and matched increase in circulating mature human neutrophils. Imaging NSG-3GS recipients of lenti-luciferase-transduced cells showed that human cells being produced 3 weeks posttransplant were heterogeneously distributed, validating the blood as a more representative measure of transplanted STRC activity. Limiting dilution transplants further demonstrated that the early increase in human granulopoiesis in NSG-3GS mice reflects an expanded output of differentiated cells per STRC rather than an increase in STRC detection.NSG-3GS mice support enhanced clonal outputs from human short-term repopulating cells (STRCs) without affecting their engrafting efficiency. Increased human STRC clone sizes enable their more precise and efficient measurement by peripheral blood monitoring.

Published

2013

37. Distinct signaling programs control human hematopoietic stem cell survival and proliferation

Author

Weijia Wang, Carl L. Hansen, Karen Sachs, Davide Pellacani, Wenlian Qiao, David J.H.F. Knapp, Guy Sauvageau, Sean C. Bendall, Philip A. Beer, Connie J. Eaves, Nima Aghaeepour, Garry P. Nolan, R. Keith Humphries, Peter W. Zandstra, Paul H. Miller, and Colin A. Hammond

Subjects

0301 basic medicine, Cell Survival, Hematopoiesis and Stem Cells, Immunology, CD34, Stem cell factor, Biology, Biochemistry, Immunophenotyping, 03 medical and health sciences, Mice, 0302 clinical medicine, medicine, Animals, Humans, CD90, Protein kinase B, Interleukin 3, Cell Proliferation, Cell growth, Hematopoietic stem cell, hemic and immune systems, Cell Biology, Hematology, Hematopoietic Stem Cells, Cell biology, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Cord blood, Intercellular Signaling Peptides and Proteins, Signal Transduction, Transcription Factors

Abstract

Several growth factors (GFs) that together promote quiescent human hematopoietic stem cell (HSC) expansion ex vivo have been identified; however, the molecular mechanisms by which these GFs regulate the survival, proliferation. and differentiation of human HSCs remain poorly understood. We now describe experiments in which we used mass cytometry to simultaneously measure multiple surface markers, transcription factors, active signaling intermediates, viability, and cell-cycle indicators in single CD34+ cord blood cells before and up to 2 hours after their stimulation with stem cell factor, Fms-like tyrosine kinase 3 ligand, interleukin-3, interleukin-6, and granulocyte colony-stimulating factor (5 GFs) either alone or combined. Cells with a CD34+CD38-CD45RA-CD90+CD49f+ (CD49f+) phenotype (∼10% HSCs with >6-month repopulating activity in immunodeficient mice) displayed rapid increases in activated STAT1/3/5, extracellular signal-regulated kinase 1/2, AKT, CREB, and S6 by 1 or more of these GFs, and β-catenin only when the 5 GFs were combined. Certain minority subsets within the CD49f+ compartment were poorly GF-responsive and, among the more GF-responsive subsets of CD49f+ cells, different signaling intermediates correlated with the levels of the myeloid- and lymphoid-associated transcription factors measured. Phenotypically similar, but CD90-CD49f- cells (MPPs) contained lower baseline levels of multiple signaling intermediates than the CD90+CD49f+ cells, but showed similar response amplitudes to the same GFs. Importantly, we found activation or inhibition of AKT and β-catenin directly altered immediate CD49f+ cell survival and proliferation. These findings identify rapid signaling events that 5 GFs elicit directly in the most primitive human hematopoietic cell types to promote their survival and proliferation.

Published

2016

38. Increasingly Successful Highly Active Antiretroviral Therapy Delays the Emergence of New HLA Class I–Associated Escape Mutations in HIV-1

Author

P. Richard Harrigan, Chanson J. Brumme, Zabrina L. Brumme, Sheng Yuan Huang, Brian Wynhoven, David J.H.F. Knapp, Winnie Dong, and Theresa Mo

Subjects

Adult, Male, Microbiology (medical), Population, Epitopes, T-Lymphocyte, HIV Infections, Drug resistance, Human leukocyte antigen, Immune system, Antiretroviral Therapy, Highly Active, Humans, Cytotoxic T cell, Medicine, Selection, Genetic, education, Immune Evasion, education.field_of_study, Polymorphism, Genetic, British Columbia, business.industry, Histocompatibility Antigens Class I, virus diseases, Viral Load, Reverse transcriptase, Infectious Diseases, pol Gene Products, Human Immunodeficiency Virus, Mutation, Cohort, Immunology, HIV-1, Female, business, Viral load, T-Lymphocytes, Cytotoxic

Abstract

Background. HLA class I–restricted cytotoxic T lymphocytes and highly active antiretroviral therapy (HAART) exert strong selective pressures on human immunodeficiency virus type 1 (HIV-1), leading to escape mutations compromising virologic control. Immune responses continue to shape HIV-1 evolution after HAART initiation, but the extent and rate at which this occurs remain incompletely quantified. Here, we characterize the incidence and clinical correlates of HLA-associated evolution in HIV-1 Pol after HAART initiation in a large, population-based observational cohort. Methods. British Columbia HAART Observational, Medical Evaluation and Research cohort participants with available HLA class I types and longitudinal posttherapy protease/reverse transcriptase sequences were studied (n 5 619; median, 5 samples per patient and 5.2 years of follow-up). HLA-associated polymorphisms were defined according to published reference lists. Rates and correlates of immune-mediated HIV-1 evolution were investigated using multivariate Cox proportional hazard models incorporating baseline and time-dependent plasma viral load and CD4 response data. Results. New HLA-associated escape events were observed in 269 (43%) patients during HAART and occurred at 49 of 63 (78%) investigated immune-associated sites in Pol. In time-dependent analyses adjusting for baseline factors, poorer virologic, but not immunologic, response to HAART was associated with increased risk of immune escape of 1.9-fold per log10 viral load increment (P , .0001). Reversion of escape mutations following HAART initiation was extremely rare. Conclusions. HLA-associated HIV-1 evolution continues during HAART to an extent that is inversely related to the virologic success of therapy. Minimizing the degree of immune escape could represent a secondary benefit of effective HAART.

Published

2012

39. Global Transcriptome Profiling Identifies a Key Mir-185-PAK6 Axis That Promotes Survival of Leukemic Stem Cells and Drug-Insensitive Blasts in BCR-ABL+ Human Leukemia

Author

Min Chen, Andrew Wu, David J.H.F. Knapp, Oleh Petriv, R. Keith Humphries, Donna L. Forrest, Kieran O'Neill, Jens Ruschmann, Katharina Rothe, Carl L. Hansen, Xiaoyan Jiang, Naoto Nakamichi, Inanc Birol, Connie J. Eaves, Tobias Maetzig, Ryan R. Brinkman, and Lin Hanyang

Subjects

Immunology, Cell Biology, Hematology, Biology, medicine.disease, Biochemistry, Transplantation, Dasatinib, Gene expression profiling, Leukemia, medicine.anatomical_structure, Acute lymphocytic leukemia, microRNA, medicine, Cancer research, Bone marrow, Stem cell, medicine.drug

Abstract

Chronic myeloid leukemia (CML) stem/progenitor cells and BCR-ABL+ acute lymphoblastic leukemia (ALL) blast cells are insensitive to tyrosine kinase inhibitor (TKI) monotherapies. These cells rapidly generate therapy-resistant clones in vitro and in vivo and are often responsible for disease relapse. Therefore, identification of predictive biomarkers and novel treatments that target key molecular events active in leukemic stem cells (LSCs) are needed. MicroRNAs (miRNAs) are small molecules that regulate the gene expression network and are highly deregulated in many cancers. Through global transcriptome profiling, we have recently identified 66 differentially expressed miRNAs in pre-treatment CD34+ stem/progenitor cells from CML patients (n=6) compared to healthy bone marrow (NBM) controls (n=3, adjusted P Disclosures No relevant conflicts of interest to declare.

Published

2018

40. Single Cell-Resolution Analysis of HSC Dysfunction in Mir-146a knockout Mice

Author

Kieran O'Neill, Joanna Wegrzyn, Connie J. Eaves, Jeremy Parker, Jennifer M Grants, David J.H.F. Knapp, Aly Karsan, Mark Boldin, Tony Hui, Martin Hirst, and Deborah Deng

Subjects

Cell growth, Immunology, Hematopoietic stem cell, Myeloid leukemia, Cell Biology, Hematology, Biology, Biochemistry, Transplantation, Haematopoiesis, medicine.anatomical_structure, Knockout mouse, medicine, Cancer research, Progenitor cell, Stem cell

Abstract

MicroRNA miR-146a is frequently depleted in myelodysplastic syndrome (MDS) and acute myeloid leukemia (AML). Loss of miR-146a may be an initiating event in tumorigenesis, as miR-146a loss in mouse models is sufficient to cause features of MDS and eventual progression to AML. To define how miR-146a loss initiates tumorigenesis, we analyzed hematopoietic stem cell (HSC) function from miR-146a knockout (KO) mice prior to onset of an overt malignant phenotype. Tracking cell division kinetics, proliferation, and differentiation of single long-term HSC (LT-HSC; EPCR+CD45+CD48-CD150+) in culture, we found evidence that miR-146a KOreduces HSC quiescence and promotes differentiating cell divisions. Our data show that miR-146a KO HSC dysfunction may stem from loss of a CD150-bright EPCR-bright sub-population, which has previously been associated with robust HSC activity. In line with this, single cell DNA methylation profiling revealed a reduction in a primitive sub-population of LT-HSCs in miR-146a KO animals. In addition, single cell LT-HSC transplants revealed a myeloid repopulation bias. As reduced HSC cell cycle quiescence has been linked to impaired HSC self-renewal upon hematopoietic stress, such as serial transplantation, we assessed the frequency of serially transplantable HSCs by performing secondary transplants with limiting dilution. Serially transplantable HSC frequency was reduced in miR-146a KO compared to wild type, suggesting impaired HSC self-renewal. Transcriptome profiling of miR-146a KO hematopoietic stem and progenitor cells identified tumor necrosis factor (TNF) signaling activation as a potential driver of HSC dysfunction. LT-HSC cell cycle quiescence and the CD150-bright EPCR-bright LT-HSC sub-population were restored in miR-146a/TNF double KO mice, suggesting that aberrant TNF signaling activation drives HSC dysfunction upon loss of miR-146a. Gene expression levels in the TNF signaling network are inversely correlated with miR-146a levels in human AML, implying that TNF signaling may similarly disrupt HSC function in miR-146a- depleted myeloid malignancies. Overall, our findings suggest that miR-146a promotes HSC cell cycle quiescence and inhibits differentiation by antagonizing TNF signaling, in order to maintain a primitive sub-population of long-term self-renewing HSCs. Disclosures Eaves: Experimental Hematology: Other: Editor of journal; StemCell Technologies Inc: Other: Wife of owner.

Published

2017

41. Molecular and biological analysis of human hematopoietic stem cells at single-cell resolution

Author

Garry P. Nolan, Gabrielle Rabu, Paul H. Miller, Michelle Moksa, A. Hui, Philip A. Beer, Carl L. Hansen, Nima Aghaeepour, R.K. Humphries, Alireza Lorzadeh, Martin Hirst, M. van Loenhout, Davide Pellacani, F. Wang, Colin A. Hammond, Michael VanInsberghe, David J.H.F. Knapp, Sean C. Bendall, and Connie J. Eaves

Subjects

0301 basic medicine, Cancer Research, Chemistry, Cell, Resolution (electron density), Cell Biology, Hematology, Cell biology, 03 medical and health sciences, Haematopoiesis, 030104 developmental biology, medicine.anatomical_structure, Genetics, medicine, Stem cell, Molecular Biology

Published

2017

42. Roles of microrna miR-146a in hematopoietic stem cell function

Author

David J.H.F. Knapp, Connie J. Eaves, Jennifer Grants, Kieran O'Neill, Deborah Deng, Aly Karsan, Tony Hui, Martin Hirst, Jeremy Parker, and Joanna Wegrzyn

Subjects

Cancer Research, medicine.anatomical_structure, microRNA, Genetics, medicine, Hematopoietic stem cell, Cell Biology, Hematology, Biology, Molecular Biology, Function (biology), Cell biology

Published

2017

43. Prevalence and Virologic Consequences of Transmitted HIV-1 Drug Resistance in Uganda

Author

Jessica H. Oyugi, John Bennett, David J.H.F. Knapp, P. Richard Harrigan, Chanson J. Brumme, Conrad Muzoora, Peter W. Hunt, Nneka Emenyonu, Yap Boum, David R. Bangsberg, Jeffrey N. Martin, and Guinevere Q. Lee

Subjects

Adult, Male, medicine.medical_specialty, Cross-sectional study, Immunology, Clinical Sciences, Human immunodeficiency virus (HIV), Drug Resistance, HIV Infections, Drug resistance, medicine.disease_cause, Polymerase Chain Reaction, Outcomes Research, Acquired immunodeficiency syndrome (AIDS), Clinical Research, Internal medicine, Virology, Drug Resistance, Viral, medicine, Prevalence, Humans, Uganda, Viral, business.industry, Evaluation of treatments and therapeutic interventions, medicine.disease, Antiretroviral therapy, Regimen, Infectious Diseases, Good Health and Well Being, Cross-Sectional Studies, 6.1 Pharmaceuticals, Cohort, HIV-1, HIV/AIDS, Female, business, Infection, Viral load

Abstract

Few reports have examined the impact of HIV-1 transmitted drug resistance (TDR) in resource-limited settings where there are fewer regimen choices and limited pretherapy/posttherapy resistance testing. In this study, we examined TDR prevalence in Kampala and Mbarara, Uganda and assessed its virologic consequences after antiretroviral therapy initiation. We sequenced the HIV-1 protease/reverse transcriptase from n=81 and n=491 treatment-naive participants of the Uganda AIDS Rural Treatment Outcomes (UARTO) pilot study in Kampala (AMU 2002-2004) and main cohort in Mbarara (MBA 2005-2010). TDR-associated mutations were defined by the WHO 2009 surveillance mutation list. Posttreatment viral load data were available for both populations. Overall TDR prevalence was 7% (Kampala) and 3% (Mbarara) with no significant time trend. There was a slight but statistically nonsignificant trend indicating that the presence of TDR was associated with a worse treatment outcome. Virologic suppression (≤400 copies/ml within 6 months posttherapy initiation) was achieved in 87% and 96% of participants with wildtype viruses versus 67% and 83% of participants with TDR (AMU, MBA p=0.2 and 0.1); time to suppression (log-rank p=0.3 and p=0.05). Overall, 85% and 96% of study participants achieved suppression regardless of TDR status. Surprisingly, among the TDR cases, approximately half still achieved suppression; the presence of pretherapy K103N while on nevirapine and fewer active drugs in the first regimen were most often observed with failures. The majority of patients benefited from the local HIV care system even without resistance monitoring. Overall, TDR prevalence was relatively low and its presence did not always imply treatment failure.

Published

2014

44. DNA barcoding reveals diverse growth kinetics of human breast tumour subclones in serially passaged xenografts

Author

Samuel Aparicio, Annaick Carles, David J.H.F. Knapp, Claire Cox, Sneha Balani, Connie J. Eaves, Sohrab P. Shah, Michelle Moksa, Martin Hirst, Nagarajan Kannan, Peter Eirew, Davide Pellacani, and Long V. Nguyen

Subjects

Multidisciplinary, Growth kinetics, General Physics and Astronomy, Breast Neoplasms, General Chemistry, Biology, Bioinformatics, DNA barcoding, General Biochemistry, Genetics and Molecular Biology, Article, Clone Cells, Kinetics, Mice, Cell Line, Tumor, Cancer cell, Cancer research, Tumor Cells, Cultured, Animals, DNA Barcoding, Taxonomic, Humans, Female, Human breast, Clonal growth, Neoplasm Transplantation, Cell Proliferation

Abstract

Genomic and phenotypic analyses indicate extensive intra- as well as intertumoral heterogeneity in primary human malignant cell populations despite their clonal origin. Cellular DNA barcoding offers a powerful and unbiased alternative to track the number and size of multiple subclones within a single human tumour xenograft and their response to continued in vivo passaging. Using this approach we find clone-initiating cell frequencies that vary from ~1/10 to ~1/10,000 cells transplanted for two human breast cancer cell lines and breast cancer xenografts derived from three different patients. For the cell lines, these frequencies are negatively affected in transplants of more than 20,000 cells. Serial transplants reveal five clonal growth patterns (unchanging, expanding, diminishing, fluctuating or of delayed onset), whose predominance is highly variable both between and within original samples. This study thus demonstrates the high growth potential and diverse growth properties of xenografted human breast cancer cells., Cancer cells within the same tumour are heterogeneous in their tumorigenic potential, differentiation status and sensitivity to treatments. Here Nguyen et al. use a sensitive DNA barcoding method to characterize the diversity of clonal growth behaviour within human breast tumours.

Published

2014

45. Dominant-negative IKAROS enhances IL-3-stimulated signaling in wild-type but not BCR-ABL1(+) mouse BA/F3 cells

Author

Nagarajan Kannan, Lisa Wei, Connie J. Eaves, Philip A. Beer, David J.H.F. Knapp, Sofia von Palffy, Elizabeth Bulaeva, and Sonja Babovic

Subjects

Gene isoform, Cancer Research, Cell Survival, Recombinant Fusion Proteins, Fusion Proteins, bcr-abl, Endogeny, Biology, 03 medical and health sciences, Ikaros Transcription Factor, Mice, 0302 clinical medicine, Transduction, Genetic, hemic and lymphatic diseases, Genetics, Animals, Humans, Cell Lineage, Myeloid Cells, Lymphocytes, Molecular Biology, Transcription factor, Cells, Cultured, 030304 developmental biology, Cell Line, Transformed, Genes, Dominant, 0303 health sciences, B-Lymphocytes, Wild type, Myeloid leukemia, Cell Biology, Hematology, Molecular biology, Phenotype, Cell Transformation, Neoplastic, Cell culture, 030220 oncology & carcinogenesis, Mutation, Interleukin-3, Intracellular, Cell Division, Signal Transduction

Abstract

Inactivating mutations in IKZF1 , the gene that encodes the transcription factor IKAROS, are recurrent in poor-prognosis human B-cell leukemias, in which these mutations co-exist with BCR-ABL1 or other genetic changes that activate similar intracellular signaling pathways. However, little is known about the mechanism(s) by which loss of IKAROS activity may co-operate with BCR-ABL1 to transform lymphoid cells. To investigate this question, we used expression of a dominant-negative isoform of IKAROS (IK6) to suppress endogenous IKAROS activity in the interleukin-3 (IL-3)-dependent mouse pro-B BA/F3 cell line and in an IL-3-independent BCR-ABL1 + derivative. We then used intracellular phospho-flow cytometry to assess the effects of BCR-ABL1 and IK6, alone and in combination, on the signaling state of the cells before and after their stimulation with IL-3. BCR-ABL1 and IK6 each produced a constitutively activated signaling phenotype and also enhanced the signaling responses of BA/F3 cells to IL-3. These effects, however, were neither equivalent nor additive, and IK6 alone was insufficient to confer the IL-3-independent growth characteristic of BCR-ABL1 + BA/F3 cells. In addition to its effects on lymphoid cells, IK6 also induced constitutively activated signaling in a subset of myeloid leukemia cell lines. Together, these studies indicate an ability of IK6 to enhance intracellular signaling in both lymphoid and myeloid cells, but not to synergize with BCR-ABL1 in this model system.

Published

2014

46. 'Deep' sequencing accuracy and reproducibility using Roche/454 technology for inferring co-receptor usage in HIV-1

Author

P. Richard Harrigan, Winnie Dong, Rachel A. McGovern, Dennison Chan, Xiaoyin Zhong, Luke C. Swenson, Art F. Y. Poon, and David J.H.F. Knapp

Subjects

Viral Diseases, Epidemiology, Human immunodeficiency virus (HIV), lcsh:Medicine, HIV Infections, medicine.disease_cause, Immunodeficiency Viruses, Statistics, Genome Sequencing, lcsh:Science, Genetics, Multidisciplinary, Antimicrobials, High-Throughput Nucleotide Sequencing, Sampling error, Genomics, Antivirals, 3. Good health, Infectious Diseases, Medical Microbiology, HIV epidemiology, Viral Pathogens, Research Article, Clinical cohort, Sequence analysis, Coefficient of variation, Biology, Microbiology, Deep sequencing, Microbial Control, Virology, medicine, Humans, Molecular Biology Techniques, Sequencing Techniques, Microbial Pathogens, Molecular Biology, Medicine and health sciences, Reproducibility, Sequence Analysis, RNA, Low input, lcsh:R, Reproducibility of Results, Biology and Life Sciences, Computational Biology, HIV, Genome Analysis, HIV-1, lcsh:Q

Abstract

Next generation, "deep", sequencing has increasing applications both clinically and in disparate fields of research. This study investigates the accuracy and reproducibility of "deep" sequencing as applied to co-receptor prediction using the V3 loop of Human Immunodeficiency Virus-1. Despite increasing use in HIV co-receptor prediction, the accuracy and reproducibility of deep sequencing technology, and the factors which can affect it, have received only a limited level of investigation. To accomplish this, repeated deep sequencing results were generated using the Roche GS-FLX (454) from a number of sources including a non-homogeneous clinical sample (N = 47 replicates over 18 deep sequencing runs), and a large clinical cohort from the MOTIVATE and A400129 studies (N = 1521). For repeated measurements of a non-homogeneous clinical sample, increasing input copy number both decreased variance in the measured proportion of non-R5 using virus (p<

Published

2013

47. Developmental changes in the in vitro activated regenerative activity of primitive mammary epithelial cells

Author

Maisam Makarem, Long V. Nguyen, Afshin Raouf, Peter Eirew, Connie J. Eaves, John Stingl, Michael D. Prater, Oksana Nemirovsky, Sneha Balani, Nagarajan Kannan, and David J.H.F. Knapp

Subjects

QH301-705.5, Cellular differentiation, Biology, General Biochemistry, Genetics and Molecular Biology, Mice, 03 medical and health sciences, Mammary Glands, Animal, 0302 clinical medicine, Cancer stem cell, Neurosphere, Animals, Biology (General), 030304 developmental biology, Stem cell transplantation for articular cartilage repair, 0303 health sciences, General Immunology and Microbiology, Stem Cells, General Neuroscience, Epithelial Cells, 3T3 Cells, Immunohistochemistry, Cell biology, Endothelial stem cell, Adult Stem Cells, 030220 oncology & carcinogenesis, Amniotic epithelial cells, Immunology, Female, Stem cell, General Agricultural and Biological Sciences, Research Article, Developmental Biology, Adult stem cell

Abstract

Mouse fetal mammary cells display greater regenerative activity than do adult mammary cells when stimulated to proliferate in a new system that supports the production of transplantable mammary stem cells ex vivo., Many normal adult tissues contain rare stem cells with extensive self-maintaining regenerative potential. During development, the stem cells of the hematopoietic and neural systems undergo intrinsically specified changes in their self-renewal potential. In the mouse, mammary stem cells with transplantable regenerative activity are first detectable a few days before birth. They share some phenotypic properties with their adult counterparts but are enriched in a subpopulation that displays a distinct gene expression profile. Here we show that fetal mammary epithelial cells have a greater direct and inducible growth potential than their adult counterparts. The latter feature is revealed in a novel culture system that enables large numbers of in vitro clonogenic progenitors as well as mammary stem cells with serially transplantable activity to be produced within 7 days from single fetal or adult input cells. We further show that these responses are highly dependent on novel factors produced by fibroblasts. These findings provide new avenues for elucidating mechanisms that regulate normal mammary epithelial stem cell properties at the single-cell level, how these change during development, and how their perturbation may contribute to transformation., Author Summary Many adult tissues are maintained by a rare subset of undifferentiated stem cells that can self-renew and give rise to specialized daughter cells that have a more limited regenerative ability. The recent identification of cells in the fetal and adult mammary gland that display the properties of stem cells provides a foundation for investigating their self-renewal and differentiation control. We now show that these stem cell properties can be elicited from single mouse mammary cells placed in 3D cultures if novel factors produced by fibroblasts are present. Moreover, a comparison of the clonal outputs of fetal and adult mammary cells in this in vitro system shows that the fetal mammary cells have superior regenerative activity relative to their adult counterparts. The ability to activate and quantify the regenerative capacity of single mouse mammary epithelial cells in vitro sets the stage for further investigations of the timing and mechanisms that alter their stem cell properties during development, the potential relevance of these events to other normal epithelial tissues, and how these processes might be involved in the genesis of breast cancer.

Published

2013

48. Correlates of Protective Cellular Immunity Revealed by Analysis of Population-Level Immune Escape Pathways in HIV-1

Author

Mark A. Brockman, Sharon A. Riddler, P. Richard Harrigan, Chanson J. Brumme, Anh Q. Le, Richard Apps, Simon Mallal, George W. Nelson, Eric Martin, Charles E. DeZiel, Zabrina L. Brumme, Jonathan M. Carlson, David J.H.F. Knapp, Celia K. S. Chui, Mina John, Jennifer Listgarten, Laura A. Cotton, Richard Haubrich, Mary Carrington, Nico Pfeifer, and David Heckerman

Subjects

Genetics, Cellular immunity, Immunity, Cellular, Immunogenicity, Immunology, Human leukocyte antigen, Biology, Microbiology, Epitope, Histocompatibility, CTL, Epitopes, Immune system, HLA Antigens, Virology, Insect Science, HIV-1, Pathogenesis and Immunity, Humans, Allele, Alleles, Immune Evasion

Abstract

HLA class I-associated polymorphisms identified at the population level mark viral sites under immune pressure by individual HLA alleles. As such, analysis of their distribution, frequency, location, statistical strength, sequence conservation, and other properties offers a unique perspective from which to identify correlates of protective cellular immunity. We analyzed HLA-associated HIV-1 subtype B polymorphisms in 1,888 treatment-naïve, chronically infected individuals using phylogenetically informed methods and identified characteristics of HLA-associated immune pressures that differentiate protective and nonprotective alleles. Over 2,100 HLA-associated HIV-1 polymorphisms were identified, approximately one-third of which occurred inside or within 3 residues of an optimally defined cytotoxic T-lymphocyte (CTL) epitope. Differential CTL escape patterns between closely related HLA alleles were common and increased with greater evolutionary distance between allele group members. Among 9-mer epitopes, mutations at HLA-specific anchor residues represented the most frequently detected escape type: these occurred nearly 2-fold more frequently than expected by chance and were computationally predicted to reduce peptide-HLA binding nearly 10-fold on average. Characteristics associated with protective HLA alleles (defined using hazard ratios for progression to AIDS from natural history cohorts) included the potential to mount broad immune selection pressures across all HIV-1 proteins except Nef, the tendency to drive multisite and/or anchor residue escape mutations within known CTL epitopes, and the ability to strongly select mutations in conserved regions within HIV's structural and functional proteins. Thus, the factors defining protective cellular immune responses may be more complex than simply targeting conserved viral regions. The results provide new information to guide vaccine design and immunogenicity studies.

Published

2012

49. Abstract A23: Human mammary luminal progenitor cells use cKIT-H2O2 interactions to regulate their growth

Author

Yifei Dong, Hequn Wang, Peter Eirew, Nagarajan Kannan, Davide Pellacani, Haishan Zeng, Kingsley Shih, Connie J. Eaves, and David J.H.F. Knapp

Subjects

Cancer Research, Matrigel, medicine.diagnostic_test, Kinase, Cell growth, Tyrosine phosphorylation, Biology, Cell biology, chemistry.chemical_compound, Oncology, Biochemistry, chemistry, Western blot, Cell surface receptor, Cancer research, medicine, Phosphorylation, Molecular Biology, Tyrosine kinase

Abstract

Hydrogen peroxides (H2O2) are known to activate multiple cell signaling pathways but the mechanisms involved and how they are differentially regulated in specific normal mammary cell types is unknown. The luminal progenitor (LP) fraction of cells of the normal human mammary gland are of particular interest in this regard because, compared to the basal cells (BCs), these cells consume more O2, sustain higher levels of ROS, and are more resistant to H2O2 levels by virtue of their repertoire of enzymes that reduce both ROS and oxidized nucleotide products of ROS. However, these features of normal human LPs are also accompanied by their accumulation of more DNA damage. Here we examine the idea that the greater tolerance of LPs to ROS may be associated with a previously unknown intracellular signaling role of ROS in these cells. Using an optimized quantitative twin-photon and confocal-reflectance imaging system, we have found that the size of the spherical 3D structures produced in Matrigel cultures by freshly isolated, FACS-purified normal human LPs is increased in the presence of exogenous H2O2 at concentrations that are toxic to BCs. In addition to LPs, co-purified non-clonogenic luminal cells (LCs) display elevated levels of peroxiredoxin-1 peroxidase, a negative regulator of H2O2 action, as compared to BCs. Both of the luminal cell types (but not BCs) also showed tyrosine phosphorylation of peroxiredoxin-1 peroxidase (a biomarker of H2O2 action) when exposed for 10 minutes to exogenous H2O2, but LPs only showed marked inactivation of peroxiredoxin-1 in the absence of an external stimulus. Western blot analysis revealed a parallel and dramatic H2O2-induced pan-tyrosine phosphorylation response selectively in both luminal subsets, and their analysis at the single cell level by mass cytometry using a CyTOF identified multiple activated signaling intermediates. From FACS, immunohistochemistry, Western blot, microarray and RNA-Seq data analyses, we identified cKIT as the most differentially and highly expressed (albeit trypsin-sensitive) tyrosine kinase in LPs. Epigenetic analysis of the cKIT promoter showed it to be in an ‘open’ state exclusively in human LPs, and H2O2 treatment alone was sufficient to rapidly activate auto-phosphorylation of the cKIT Y719 residue, a site known to bind and thereby lead to the activation of PI3 kinase. Taken together, these findings reveal a new, ligand-independent function of a cell surface receptor in mediating a potent, lineage-specific signaling function of H2O2 that, in normal human mammary cells influences cell growth. Citation Format: Nagarajan Kannan, Kingsley Shih, Yifei Dong, Peter Eirew, David Knapp, Davide Pellacani, Hequn Wang, Haishan Zeng, Connie Eaves. Human mammary luminal progenitor cells use cKIT-H2O2 interactions to regulate their growth. [abstract]. In: Proceedings of the AACR Special Conference on Advances in Breast Cancer Research; Oct 17-20, 2015; Bellevue, WA. Philadelphia (PA): AACR; Mol Cancer Res 2016;14(2_Suppl):Abstract nr A23.

Published

2016

50. The Lin28b-let-7-Hmga2 axis determines the higher self-renewal potential of fetal haematopoietic stem cells

Author

Florian Kuchenbauer, Sonja Babovic, David G. Kent, David J.H.F. Knapp, Michael R. Copley, Christopher Day, Philip A. Beer, Claudia Benz, R. Keith Humphries, Connie J. Eaves, Stefan Wöhrer, Heidi Mader, Keegan Rowe, and David Q. Treloar

Subjects

Cell signaling, Cellular differentiation, Biology, LIN28, Polymerase Chain Reaction, Mice, Fetus, Downregulation and upregulation, Animals, Lymphocytes, Cell Proliferation, Oligonucleotide Array Sequence Analysis, Regulation of gene expression, Mice, Knockout, HMGA2 Protein, Gene Expression Regulation, Developmental, RNA-Binding Proteins, hemic and immune systems, Cell Differentiation, Cell Biology, Flow Cytometry, Hematopoietic Stem Cells, Cell biology, Up-Regulation, DNA-Binding Proteins, Mice, Inbred C57BL, Haematopoiesis, MicroRNAs, Animals, Newborn, Stem cell, Signal Transduction

Abstract

Mouse haematopoietic stem cells (HSCs) undergo a postnatal transition in several properties, including a marked reduction in their self-renewal activity. We now show that the developmentally timed change in this key function of HSCs is associated with their decreased expression of Lin28b and an accompanying increase in their let-7 microRNA levels. Lentivirus-mediated overexpression of Lin28 in adult HSCs elevates their self-renewal activity in transplanted irradiated hosts, as does overexpression of Hmga2, a well-established let-7 target that is upregulated in fetal HSCs. Conversely, HSCs from fetal Hmga2−/− mice do not exhibit the heightened self-renewal activity that is characteristic of wild-type fetal HSCs. Interestingly, overexpression of Hmga2 in adult HSCs does not mimic the ability of elevated Lin28 to activate a fetal lymphoid differentiation program. Thus, Lin28b may act as a master regulator of developmentally timed changes in HSC programs with Hmga2 serving as its specific downstream modulator of HSC self-renewal potential. Fetal haematopoietic stem cells (HSCs) display higher self-renewal potential than their adult counterparts. Eaves and colleagues show that adult HSCs express lower levels of Lin28b and higher levels of let-7 miRNA. They demonstrate that Lin28 overexpression, as well as that of Hmga2 (a target of let-7), induces fetal properties in adult HSCs. Conversely, HMGA2 loss in fetal HSCs results in premature induction of adult HSC self-renewal properties.

Published

2012