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  • New NIH study reveals shared genetic mar

    From ScienceDaily@1:317/3 to All on Wed Mar 22 22:30:26 2023
    New NIH study reveals shared genetic markers underlying substance use disorders
    Breakthrough findings could lead to more effective prevention and
    treatment strategies for multiple substance use disorders

    Date:
    March 22, 2023
    Source:
    NIH/National Institute on Drug Abuse
    Summary:
    By combing through genomic data of over 1 million people of
    European or African descent, scientists have identified genes
    commonly inherited across addiction disorders, regardless of
    the substance being used. This dataset -- one of largest and most
    diverse of its kind -- may help reveal new treatment targets across
    multiple substance use disorders, including for people diagnosed
    with more than one. The findings also reinforce the role of the
    dopamine system in addiction, by showing that the combination
    of genes underlying addiction disorders was also associated with
    regulation of dopamine signaling.


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    FULL STORY ==========================================================================
    By combing through genomic data of over 1 million people, scientists have identified genes commonly inherited across addiction disorders, regardless
    of the substance being used. This dataset -- one of the largest of its
    kind -- may help reveal new treatment targets across multiple substance
    use disorders, including for people diagnosed with more than one. The
    findings also reinforce the role of the dopamine system in addiction,
    by showing that the combination of genes underlying addiction disorders
    was also associated with regulation of dopamine signaling.


    ========================================================================== Published today in Nature Mental Health, the study was led by researchers
    at the Washington University in St. Louis, along with more than 150
    coauthors from around the world. It was supported by the National
    Institute on Drug Abuse (NIDA), the National Institute on Alcohol Abuse
    and Alcoholism (NIAAA), the National Institute of Mental Health (NIMH),
    the Eunice Kennedy Shriver National Institute of Child Health and Human Development, and the National Institute on Aging.

    There has been limited knowledge of the molecular genetic underpinnings of addiction until now. Further, most clinical trials and behavioral studies
    have focused on individual substances, rather than addiction more broadly.

    Genetics play a key role in determining health throughout our lives,
    but they are not destiny. Our hope with genomic studies is to further illuminate factors that may protect or predispose a person to substance
    use disorders -- knowledge that can be used to expand preventative
    services and empower individuals to make informed decisions about drug
    use," said NIDA Director, Nora Volkow, M.D.

    "A better understanding of genetics also brings us one step closer to developing personalized interventions that are tailored to an individual's unique biology, environment, and lived experience in order to provide
    the most benefits." In 2021, more than 46 million people in the United
    States aged 12 or older had at least one substance use disorder, and
    only 6.3% had received treatment.

    Moreover, people who use drugs are facing an increasingly dangerous
    drug supply, now often tainted with fentanyl. Approximately 107,000
    people died of drug overdoses in 2021, and 37% of these deaths involved simultaneous exposure to both opioids and stimulant drugs. Drug use and addiction represent a public health crisis, characterized by high social, emotional, and financial costs to families, communities, and society.

    Substance use disorders are heritable and influenced by complex
    interactions among multiple genes and environmental factors. In recent
    decades, a data-rich method, called genome-wide association, has emerged
    to try to identify specific genes involved in certain disorders. This
    method involves searching entire genomes for regions of genetic variation, called single-nucleotide polymorphisms (SNPs), that associate with the
    same disease, disorder, condition, or behavior among multiple people.

    In this study, researchers used this method to pinpoint areas in the
    genome associated with general addiction risk, as well as the risk of
    specific substance use disorders -- namely, alcohol, nicotine, cannabis,
    and opioid use disorders -- in a sample of 1,025,550 individuals with
    genes indicating European ancestry and 92,630 individuals with genes
    indicating African ancestry.

    "Using genomics, we can create a data-driven pipeline to prioritize
    existing medications for further study and improve chances of discovering
    new treatments. To do this accurately, it's critical that the genetic
    evidence we gather includes globally representative populations and
    that we have members of communities historically underrepresented in
    biomedical research leading and contributing to these kinds of studies,"
    said Alexander Hatoum, Ph.D., a research assistant professor at Washington University in St. Louis and lead author of the study.

    Hatoum and the research team discovered various molecular patterns
    underlying addiction, including 19 independent SNPs significantly
    associated with general addiction risk and 47 SNPs for specific substance disorders among the European ancestry sample. The strongest gene signals consistent across the various disorders mapped to areas in the genome
    known to control regulation of dopamine signaling, suggesting that
    genetic variation in dopamine signaling regulation, rather than in
    dopamine signaling itself, is central to addiction risk.

    Compared to other genetic predictors, the genomic pattern identified here
    was also a more sensitive predictor of having two or more substance
    use disorders at once. The genomic pattern also predicted higher
    risk of mental and physical illness, including psychiatric disorders,
    suicidal behavior, respiratory disease, heart disease, and chronic pain conditions. In children aged 9 or 10 years without any experience of
    substance use, these genes correlated with parental substance use and externalizing behavior.

    "Substance use disorders and mental disorders often co-occur, and we
    know that the most effective treatments help people address both issues
    at the same time.

    The shared genetic mechanisms between substance use and mental disorders revealed in this study underscore the importance of thinking about these disorders in tandem," said NIMH Director Joshua A. Gordon, M.D., Ph.D.

    Genomic analysis in the African ancestry sample revealed one SNP
    associated with general addiction risk and one substance-specific SNP for
    risk of alcohol use disorder. The dearth of findings here underscores
    ongoing disparities in data inclusion of globally representative
    populations that must be addressed to ensure data robustness and accuracy, Hatoum and co-authors note.

    The inclusion of data from different ancestral groups in this study cannot
    and should not be used to assign or categorize variable genetic risk for substance use disorder to specific populations. As genetic information
    is used to better understand human health and health inequities,
    expansive and inclusive data collection is essential. NIDA and other
    Institutes at NIH supported a recently released report on responsible
    use and interpretation of population-level genomic data by the National Academies of Sciences, Engineering, and Medicine.

    While Hatoum and colleagues have identified a genetic pattern indicating
    broad addiction risk, they note that substance use-specific diagnoses
    still have meaning. "The current study validates previous findings of alcohol-specific risk variants, and, importantly, makes this finding in
    a very large and more diverse study population," said NIAAA Director
    George F. Koob, Ph.D. "The finding of shared genetic risk variants
    across different substance use disorders provides insight into some of
    the mechanisms that underlie these disorders and the relationships with
    other mental health conditions. Together the findings of alcohol-specific
    risk variants and common addiction-related variants provide powerful
    support for individualized prevention and treatment." This study was
    supported by multiple grants: NIDA (T32DA007261, DA054869, R01DA054750, K02DA032573, U01DA055367, K01DA051759, DP1DA054394, R33DA047527); NIAAA (K01AA030083, R21AA027827, R01AA027522, F31AA029934, T32AA028259); NIMH (K23MH121792, T32MH014276, R01MH120219); NIA (RF1AG073593, P30AG066614);
    NICHD (P2CHD042849)
    * RELATED_TOPICS
    o Health_&_Medicine
    # Personalized_Medicine # Controlled_Substances #
    Diseases_and_Conditions # Mental_Health_Research
    o Mind_&_Brain
    # Addiction # Illegal_Drugs # Disorders_and_Syndromes #
    Mental_Health
    * RELATED_TERMS
    o Addiction o Drug_addiction o Alcoholism o Dopamine o
    Sleep_disorder o Mental_illness o Personality_disorder o
    Dopamine_hypothesis_of_schizophrenia

    ========================================================================== Story Source: Materials provided by
    NIH/National_Institute_on_Drug_Abuse. Note: Content may be edited for
    style and length.


    ========================================================================== Journal Reference:
    1. Alexander S. Hatoum, Sarah M. C. Colbert, Emma C. Johnson,
    Spencer B.

    Huggett, Joseph D. Deak, Gita A. Pathak, Mariela V. Jennings,
    Sarah E.

    Paul, Nicole R. Karcher, Isabella Hansen, David A. A. Baranger,
    Alexis Edwards, Andrew D. Grotzinger, Daniel E. Adkins, Amy
    E. Adkins, Mervi Alanne-Kinnunen, Jeffry C. Alexander, Fazil Aliev,
    Silviu-Alin Bacanu, Anthony Batzler, Joanna M. Biernacka, Laura
    J. Bierut, Tim B. Bigdeli, Anna Blagonravova, Jason D. Boardman,
    Joseph M. Boden, Dorret I. Boomsma, Sandra A. Brown, Kathleen
    K. Bucholz, Danfeng Chen, Li-Shiun Chen, Doo- Sup Choi, S. Patricia
    Chou, Sven Cichon, William E. Copeland, Robin P.

    Corley, Franziska Degenhardt, Marta Di Forti, Nancy Diazgranados,
    Danielle M. Dick, Benjamin W. Domingue, Johan G. Eriksson,
    Lindsay A.

    Farrer, Jerome C. Foo, Tatiana M. Foroud, Louis Fox, Josef Frank,
    Mark A.

    Frye, Wolfgang Gaebel, Raul R. Gainetdinov, Ina Giegling, Nathan A.

    Gillespie, Alison M. Goate, David Goldman, Scott Gordon, Laura
    M. Hack, Dana B. Hancock, Kathleen Mullan Harris, Annette
    M. Hartmann, Andrew C.

    Heath, Stefanie Heilmann-Heimbach, Stefan Herms, Victor Hesselbrock,
    John K. Hewitt, Ian Hickie, Colin Hodgkinson, Per Hoffmann,
    Christian Hopfer, John Horwood, Jouke Jan Hottenga, Daniel Patrick
    Howrigan, William G.

    Iacono, Marcus Ising, Eric O. Johnson, Jaakko Kaprio, Victor
    M. Karpyak, Kenneth S. Kendler, Martin A. Kennedy, Margaret Keyes,
    Alexander Kibitov, Falk Kiefer, Bettina Konte, John Kramer,
    Kenneth Krauter, Evgeny M.

    Krupitsky, Samuel Kuperman, Jari Lahti, Marius Lahti-Pulkkinen,
    Dongbing Lai, Anastasia Levchenko, Lannie Ligthart, Penelope
    A. Lind, Susanne Lucae, Michael T. Lynskey, Pamela A. F. Madden,
    Hermine H. Maes, Patrik K. E. Magnusson, Brion S. Maher, Karl Mann,
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    Martin, Hamdi Mbarek, Matt McGue, Matthew B. McQueen, Sarah
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    Nurnberger, Aarno Palotie, Teemu Palviainen, John F. Pearson,
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    Porjesz, Ulrich W. Preuss, Diego Quattrone, Katri Ra"ikko"nen,
    Maureen D.

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    Brien P.

    Riley, Samuli Ripatti, Richard J. Rose, Dan Rujescu, Ksenia
    V. Rybakova, Euijung Ryu, Nancy L. Saccone, Jessica E. Salvatore,
    Norbert Scherbaum, Marc A. Schuckit, Melanie Schwandt, Pei-Hong
    Shen, Richard Sherva, Judy Silberg, Michael C. Stallings,
    Dan J. Stein, Fabian Streit, Jana Strohmaier, Ralph E. Tarter,
    Nathaniel Thomas, Michael M. Vanyukov, Scott Vrieze, Tamara L. Wall,
    Raymond K. Walters, Bradley T. Webb, Robbee Wedow, Frank Wendt,
    Leah Wetherill, John B. Whitfield, Stephanie Witt, Norbert Wodarz,
    Margaret J. Wright, Sarah M. Hartz, Stephanie Zellers, Haitao Zhang,
    Hongyu Zhao, Hang Zhou, Peter Zill, Lea Zillich, Elliot M.

    Tucker-Drob, Henry R. Kranzler, Lea K. Davis, Sandra Sanchez-Roige,
    Renato Polimanti, Joel Gelernter, Howard J. Edenberg, Ryan Bogdan,
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    of over 1 million subjects identifies loci underlying multiple
    substance use disorders. Nature Mental Health, 2023; 1 (3): 210 DOI:
    10.1038/s44220- 023-00034-y ==========================================================================

    Link to news story: https://www.sciencedaily.com/releases/2023/03/230322140341.htm

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