Your search keyword '"Love KS"' showing total 7 results

1. Programmable promoter editing for precise control of transgene expression.

Author

Kabaria SR, Bae Y, Ehmann ME, Beitz AM, Lende-Dorn BA, Peterman EL, Love KS, Ploessl DS, and Galloway KE

Abstract

Subtle changes in gene expression direct cells to distinct cellular states. Identifying and controlling dose-dependent transgenes require tools for precisely titrating expression. To this end, we developed a highly modular, extensible framework called DIAL for building editable promoters that allow for fine-scale, heritable changes in transgene expression. Using DIAL, we increase expression by recombinase-mediated excision of spacers between the binding sites of a synthetic zinc finger transcription factor and the core promoter. By nesting varying numbers and lengths of spacers, DIAL generates a tunable range of unimodal setpoints from a single promoter. Through small-molecule control of transcription factors and recombinases, DIAL supports temporally defined, user-guided control of transgene expression that is extensible to additional transcription factors. Lentiviral delivery of DIAL generates multiple setpoints in primary cells and iPSCs. As promoter editing generates stable states, DIAL setpoints are heritable, facilitating mapping of transgene levels to phenotypes. The DIAL framework opens new opportunities for tailoring transgene expression and improving the predictability and performance of gene circuits across diverse applications., Competing Interests: DECLARATION OF INTERESTS Patent applications related to this work have been filed by the Massachusetts Institute of Technology.

Published

2024

2. Model-guided design of microRNA-based gene circuits supports precise dosage of transgenic cargoes into diverse primary cells.

Author

Love KS, Johnstone CP, Peterman EL, Gaglione S, and Galloway KE

Abstract

To realize the potential of engineered cells in therapeutic applications, transgenes must be expressed within the window of therapeutic efficacy. Differences in copy number and other sources of extrinsic noise generate variance in transgene expression and limit the performance of synthetic gene circuits. In a therapeutic context, supraphysiological expression of transgenes can compromise engineered phenotypes and lead to toxicity. To ensure a narrow range of transgene expression, we design and characterize Co mpact m icroRNA- M ediated A ttenuator of N oise and D osage ( ComMAND ), a single-transcript, microRNA-based incoherent feedforward loop. We experimentally tune the ComMAND output profile, and we model the system to explore additional tuning strategies. By comparing ComMAND to two-gene implementations, we highlight the precise control afforded by the single-transcript architecture, particularly at relatively low copy numbers. We show that ComMAND tightly regulates transgene expression from lentiviruses and precisely controls expression in primary human T cells, primary rat neurons, primary mouse embryonic fibroblasts, and human induced pluripotent stem cells. Finally, ComMAND effectively sets levels of the clinically relevant transgenes FMRP1 and FXN within a narrow window. Together, ComMAND is a compact tool well-suited to precisely specify expression of therapeutic cargoes., Competing Interests: Declaration of Interests There are no competing interests to declare.

Published

2024

3. The sound of silence: Transgene silencing in mammalian cell engineering.

Author

Cabrera A, Edelstein HI, Glykofrydis F, Love KS, Palacios S, Tycko J, Zhang M, Lensch S, Shields CE, Livingston M, Weiss R, Zhao H, Haynes KA, Morsut L, Chen YY, Khalil AS, Wong WW, Collins JJ, Rosser SJ, Polizzi K, Elowitz MB, Fussenegger M, Hilton IB, Leonard JN, Bintu L, Galloway KE, and Deans TL

Subjects

Animals, Transgenes genetics, Cell Communication, Mammals genetics, Genetic Engineering, Gene Regulatory Networks

Abstract

To elucidate principles operating in native biological systems and to develop novel biotechnologies, synthetic biology aims to build and integrate synthetic gene circuits within native transcriptional networks. The utility of synthetic gene circuits for cell engineering relies on the ability to control the expression of all constituent transgene components. Transgene silencing, defined as the loss of expression over time, persists as an obstacle for engineering primary cells and stem cells with transgenic cargos. In this review, we highlight the challenge that transgene silencing poses to the robust engineering of mammalian cells, outline potential molecular mechanisms of silencing, and present approaches for preventing transgene silencing. We conclude with a perspective identifying future research directions for improving the performance of synthetic gene circuits., Competing Interests: Declaration of interests J.T. and L.B. acknowledge outside interest in Stylus Medicine., (Copyright © 2022 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2022

4. Scalable biological signal recording in mammalian cells using Cas12a base editors.

Author

Kempton HR, Love KS, Guo LY, and Qi LS

Subjects

Animals, Gene Editing, Humans, Mammals, RNA, Guide, CRISPR-Cas Systems, CRISPR-Cas Systems

Abstract

Biological signal recording enables the study of molecular inputs experienced throughout cellular history. However, current methods are limited in their ability to scale up beyond a single signal in mammalian contexts. Here, we develop an approach using a hyper-efficient dCas12a base editor for multi-signal parallel recording in human cells. We link signals of interest to expression of guide RNAs to catalyze specific nucleotide conversions as a permanent record, enabled by Cas12's guide-processing abilities. We show this approach is plug-and-play with diverse biologically relevant inputs and extend it for more sophisticated applications, including recording of time-delimited events and history of chimeric antigen receptor T cells' antigen exposure. We also demonstrate efficient recording of up to four signals in parallel on an endogenous safe-harbor locus. This work provides a versatile platform for scalable recording of signals of interest for a variety of biological applications., (© 2022. The Author(s), under exclusive licence to Springer Nature America, Inc.)

Published

2022

5. Multiple Input Sensing and Signal Integration Using a Split Cas12a System.

Author

Kempton HR, Goudy LE, Love KS, and Qi LS

Subjects

Breast Neoplasms genetics, Breast Neoplasms therapy, Cell Line, Tumor, Dimerization, Female, HEK293 Cells, Humans, Transcriptional Activation, CRISPR-Associated Proteins, CRISPR-Cas Systems, Cell Engineering

Abstract

The ability to integrate biological signals and execute a functional response when appropriate is critical for sophisticated cell engineering using synthetic biology. Although the CRISPR-Cas system has been harnessed for synthetic manipulation of the genome, it has not been fully utilized for complex environmental signal sensing, integration, and actuation. Here, we develop a split dCas12a platform and show that it allows for the construction of multi-input, multi-output logic circuits in mammalian cells. The system is highly programmable and can generate expandable AND gates with two, three, and four inputs. It can also incorporate NOT logic by using anti-CRISPR proteins as an OFF switch. By coupling the split dCas12a design to multiple tumor-relevant promoters, we provide a proof of concept that the system can implement logic gating to specifically detect breast cancer cells and execute therapeutic immunomodulatory responses., Competing Interests: Declaration of Interests The authors filed a provisional patent related to this work., (Copyright © 2020 Elsevier Inc. All rights reserved.)

Published

2020

6. IFN-gamma-stimulated enhancement of MHC class II antigen expression by the human mast cell line HMC-1.

Author

Love KS, Lakshmanan RR, Butterfield JH, and Fox CC

Subjects

Antigens, CD biosynthesis, B7-1 Antigen biosynthesis, B7-2 Antigen, HLA-D Antigens drug effects, Humans, Intercellular Adhesion Molecule-1 biosynthesis, Interleukin-4 pharmacology, Leukemia, Mast-Cell immunology, Leukemia, Mast-Cell metabolism, Mast Cells drug effects, Membrane Glycoproteins biosynthesis, Recombinant Proteins pharmacology, Tumor Cells, Cultured, HLA-D Antigens biosynthesis, Interferon-gamma pharmacology, Mast Cells immunology, Mast Cells metabolism

Abstract

The expression of MHC class II molecules by human mast cells has been reported in immunohistochemical surveys of inflammatory conditions, such as in tuberculin hypersensitivity. While these data suggest that human mast cells may act as antigen-presenting cells under inflammatory conditions, the induction of class II antigens on human mast cells has not been examined. In this study, we determined the effects of the inflammatory cytokines IFN-gamma and IL-4 on the expression of class II antigens HLA-DR, -DP, and -DQ by the human mast cell line HMC-1. HMC-1 cells were incubated with or without 1000 U/ml recombinant human IFN-gamma (rhIFN-gamma) and IL-4 (rhIL-4) for 72 hr and analyzed for expression of MHC class II antigens by direct immunofluorescence and flow cytometry. HMC-1 cells expressed significant levels of HLA-DR and moderate levels of HLA-DP and -DQ at baseline and when cultured without exogenous cytokines. Stimulation by rhIFN-gamma for 72 hr significantly increased the levels of HLA-DR and -DP expression but did not affect levels of HLA-DQ. Stimulation by rhIL-4 for 72 hr had minimal effect on expression of class II molecules, but induced a significant difference in levels of ICAM-1 (CD54) expression, indicating that this cytokine is involved instead in the control of certain accessory molecules. Our data showing constitutive expression of MHC class II molecules on HMC-1 cells and upregulation of that expression by rhIFN-gamma suggest that human mast cells function as antigen-presenting cells at sites where inflammatory cytokines are present.

Published

1996

7. GASEOUS LOSSES OF NITROGEN FROM GREEN PLANTS. I. STUDIES WITH CHLORELLA AND LEMNA.

Author

Allison FE, Love KS, Pinck LA, and Gaddy VL

Published

1948