281 research outputs found

    2018 Town of Shapleigh Maine Annual Town Warrant

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    Town of Shapleigh Maine Comprehensive Plan

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    Town of Shapleigh Maine Ordinances

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    2019 Town of Shapleigh Maine Annual Town Warrant

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    Town of Shapleigh Maine Audited Financial Report for the Year Ending December 31, 2018

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    Town of Shapleigh Maine 2017 Annual Report

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    Alien Registration- Shapleigh, Marie E. (Bangor, Penobscot County)

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    https://digitalmaine.com/alien_docs/10818/thumbnail.jp

    Introduction to the direct method of teaching German

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    Thesis (M.A.)--Boston University, 1917. This item was digitized by the Internet Archive

    CRISPR/Cas-based screening of long non-coding RNAs (lncRNAs) in macrophages with an NF-κB reporter.

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    The innate immune system protects against infections by initiating an inducible inflammatory response. NF-κB is one of the critical transcription factors controlling this complex response, but some aspects of its regulation remain unclear. For example, although long non-coding RNAs (lncRNAs) have been shown to critically regulate gene expression, only a fraction of these have been functionally characterized, and the extent to which lncRNAs control NF-κB expression is unknown. Here, we describe the generation of a GFP-based NF-κB reporter system in immortalized murine bone marrow-derived macrophages (iBMDM). Activation of this reporter, using Toll-like receptor ligands, resulted in GFP expression, which could be monitored by flow cytometry. We also established a CRISPR/Cas9 gene deletion system in this NF-κB reporter line, enabling us to screen for genes that regulate NF-κB signaling. Our deletion-based approach identified two long intergenic non-coding(linc)RNAs, lincRNA-Cox2 and lincRNA-AK170409, that control NF-κB signaling. We demonstrate a potential novel role for lincRNA-Cox2 in promoting IκBα degradation in the cytoplasm. For lincRNA-AK170409, we provide evidence that this nuclearly-localized lincRNA regulates a number of inflammation-related genes. In conclusion, we have established an NF-κB-GFP iBMDM reporter cell line and a line that stably expresses Cas9. Our approach enabled the identification of lincRNA-Cox2 and lincRNA-AK170409 as NF-κB regulators, and this tool will be useful for identifying additional genes involved in regulating this transcription factor critical for immune function
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