Dollars for Profs

Dig Into University Researchers' Outside Income and Conflicts of Interest

Published Dec. 6, 2019

This database was last updated in December 2019 and should only be used as a historical snapshot. There may be new or amended records not reflected here.

Financial doc
Filing Type

Conflict of Interest

Institutions must file significant disclosures to the National Institutes of Health if they determine financial relationships could affect the design, conduct or reporting of the NIH-funded research. The NIH provided us with their entire financial conflict of interest database, with filings from 2012 through 2019.

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Tom Tuschl

Rockefeller University, Department: Genetics

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Disclosed Conflict of Interest with

Regulus Therapeutics

Disclosed Value
Listed Reason
Reimbursed or sponsored travel

These grant projects could provide Regulus information about novel biomarkers used for diagnosis of diseases. Regulus' company strategy includes identifying biomarkers.

Listed Research Project
Definition of Serum Ribonucleoprotein Composition and its Regulation and Function

This application has the potential to allow us to come to a molecular understanding of the triggers of SLE and possibly other autoimmune diseases. The role of stress-induced RNA- and RBP-containing cytoplasmic granules may also reveal molecular aspects that may contribute to their deposition in inclusion bodies and amyloids in myopathies and neurodegenerative diseases. Our approach may also benchmark future developments of RNA as biomarkers and may discovery of previously unknown RNA secretory mechanism. DESCRIPTION (provided by applicant): Extracellular RNA (exRNA) from pathogens plays a key role as activator of innate immunity in mammals. However, the presence of host exRNA in serum and other body fluids challenges the current models of RNA based immune recognition. To understand its basis of specificity, it is important to catalog host exRNAs and their associated proteins in serum, investigate mechanisms leading to circulating ribonucleoprotein (RNP) homeostasis, and identify protein factors contributing to cellular RNA release. Genetic alterations in RNA targets or interacting proteins may contribute to imbalances in normal versus stress-triggered release of RNPs and push adaptive long-term pathogen-directed immunity towards autoimmunity. ExRNAs may also play a broader role in extracellular signaling similar to peptide hormones, which would also be captured by this experimental approach. This application brings together a team of multiple investigators with complementary expertise and history of close collaboration to build a solid foundation regarding identification, mechanism and function of extracellular RNAs and the proteins involved in their biogenesis, export, recognition, and turnover. The specific aims of the proposed project are: 1. Catalogue and quantify all classes of extracellular RNAs in human serum from normal subjects using various established and novel RNA seq approaches and examine normal variability of circulating RNA profiles within an individual, between individuals and the influence of gender, age, race, and disease. Establish a core facility for processing and archiving clinical materials (Williams, Putterman, Tuschi). 2. Determine exRNA composition in patients suffering from systemic lupus erythematosus (SLE), for whom antibodies against different classes of RBPs is a hallmark. Considering that these RBPs alter their subcellular localization upon stress and appear in stress granules with immature RNA and/or RNA targeted for turnover, we will evaluate in as much the composition of RNPs in stress granules harvested from immortalized B cells of normal and SLE subjects possesses immunostimulatory function and if these RNP granules are also released during stress (Tuschi, Putterman, Williams). 3. Develop a molecular and mechanistic understanding of stress granule formation and RNA/RNP mediated innate immune responses. Identify the RNA targets and RNP structures of autoantigens in tRNA stress responses, their turnover, and their immune receptors.

Filed on August 09, 2013.

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Name Institution Type Company Disclosed Value
Tom Tuschl Rockefeller University Conflict of Interest Regulus Therapeutics $0 - $4,999
Tom Tuschl Rockefeller University Conflict of Interest Regulus Therapeutics $20,000 - $39,999
Tom Tuschl Rockefeller University Conflict of Interest Regulus Therapeutics $100,000 - $149,999
Tom Tuschl Rockefeller University Conflict of Interest Regulus Therapeutics $100,000 - $149,999
Tom Tuschl Rockefeller University Conflict of Interest Regulus Therapeutics $20,000 - $39,999
Tom Tuschl Rockefeller University Conflict of Interest Max Planck $10,000 - $19,999
Tom Tuschl Rockefeller University Conflict of Interest Max Planck $10,000 - $19,999
If you see an error in the database or a reason we should not disclose a record, please contact us at [email protected] and we'll evaluate it on a case-by-case basis.
Sources: National Institutes of Health, public records requests filed at multiple public state universities

Notes: When a more specific filing date is not available for an individual financial disclosure or conflict of interest form, we use the year the form was filed. If the year was not disclosed, we report the range of years covered by our public records requests. In a few cases, a start date was provided instead of a filing date. In those cases, we use the start date instead.

Fewer than 10% of records from the University of Florida and fewer than 1% of records from the University of Texas system were removed because they did not contain enough information.

ProPublica obtained additional financial disclosures and conflict of interest forms that we have not yet digitized and added to the database. You can download those disclosures in the ProPublica Data Store.

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