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  • The immune system is very complicated, b

    From ScienceDaily@1:317/3 to All on Tue Mar 15 22:30:44 2022
    The immune system is very complicated, but now, it's on a chip
    Lymphoid follicles formed in a microfluidic Organ Chip replicate human
    immune functions and vaccine responses in vitro

    Date:
    March 15, 2022
    Source:
    Wyss Institute for Biologically Inspired Engineering at Harvard
    Summary:
    Scientists have a new tool to help them tease out the immune
    system's mysteries. Researchers cultured human B and T cells
    inside a microfluidic Organ Chip and coaxed them to form functional
    lymphoid follicles (LFs) - - structures that reside in lymph nodes
    and other parts of the human body and mediate immune responses. The
    LF Chip replicated human immune responses to both pathogens and
    a commercial influenza vaccine in vitro, offering significant
    improvement over existing preclinical models like cells in a dish
    and non-human primates.



    FULL STORY ==========================================================================
    To quote veteran science writer Ed Yong's simple yet extremely accurate
    words in The Atlantic, "The immune system is very complicated." As the
    COVID-19 pandemic had made abundantly clear, science still doesn't fully understand the sophisticated defense mechanisms that protect us from
    microbe invaders. Why do some people show no symptoms when infected with SARS-CoV-2 while others suffer from severe fevers and body aches? Why
    do some succumb to cytokine storms of the body's own making? We still
    lack exact answers to these questions.


    ========================================================================== Today's scientists, however, now have a new tool to help them tease
    out the immune system's mysteries, thanks to a group of researchers at
    the Wyss Institute for Biologically Inspired Engineering at Harvard
    University. They cultured human B and T cells inside a microfluidic
    Organ Chip device and coaxed them to spontaneously form functional
    lymphoid follicles -- structures that reside in lymph nodes and other
    parts of the human body which mediate immune responses. They consist
    of different chambers that harbor "nai"ve" B cells and T cells, which
    together initiate the cascade of events that leads to a full immune
    response when they are exposed to a specific antigen.

    In addition to allowing researchers to probe the normal function of the
    immune system, these lymphoid follicle (LF) Chips can also be used to
    predict immune responses to various vaccines and help select the best performers, offering significant improvement over existing preclinical
    models like cells in a dish and non-human primates. The achievement is
    reported today in Advanced Science.

    "Animals have been the gold-standard research models for developing and
    testing new vaccines, but their immune systems differ significantly from
    our own and do not accurately predict how humans will respond to them. Our
    LF Chip offers a way to model the complex choreography of human immune responses to infection and vaccination, and could significantly speed up
    the pace and quality of vaccine creation in the future," said first author Girija Goyal, Ph.D., a Senior Staff Scientist at the Wyss Institute.

    An accidental discovery Like many great scientific discoveries, the LF
    Chip project is the result of serendipity in the lab. Goyal and other Wyss Institute scientists wanted to investigate how B and T cells circulating
    in the blood would change their behavior once they entered a tissue,
    so they obtained those cells from human blood samples and cultured
    them inside a microfluidic Organ Chip device to replicate the physical conditions they would experience when they encountered an organ.



    ==========================================================================
    When the cells were placed inside one of the two channels within the
    device, nothing remarkable happened -- but when the researchers started
    the flow of culture medium through the other channel to feed the cells,
    they were surprised to see that the B and T cells started to spontaneously self-organize into 3D structures within the Organ Chip that appeared
    similar to "germinal centers" - - structures within LFs where complex
    immune reactions take place. "It was so unexpected that we completely
    pivoted from the original experiment and focused on trying to figure
    out what they were," said Goyal.

    When the researchers started probing the mysterious structures that had
    formed inside the Organ Chip under flow conditions, they found that the
    cells were secreting a chemical called CXCL13. CXCL13 is a hallmark of
    LF formation, both within lymph nodes and in other parts of the body
    in response to chronic inflammation, such as in cancer and autoimmune conditions.

    The team also found that B cells within the LFs that self-assembled
    on-chip also expressed an enzyme called activation-induced cytidine
    deaminase (AID), which is critical for activating B cells against specific antigens and is not present in B cells that are circulating in the blood.

    Neither CXCL13 nor AID were present in cells that were cultured in a
    standard 2D dish, suggesting that the scientists had indeed successfully created functional LFs from circulating blood cells.

    In LFs in the human body, activated B cells mature and differentiate
    into multiple types of progeny cells including plasma cells, which
    secrete large amounts of antibodies against a specific pathogen. The
    team detected the presence of plasma cells in the LF Chips after they
    applied several stimuli used in the laboratory to activate B cells,
    such as the combination of the cytokine IL-4 and an anti-CD40 antibody,
    or dead bacteria. Remarkably, the plasma cells were concentrated in
    clusters within the LFs, as they would be in vivo.

    "These findings were especially exciting because they confirmed that
    we had a functional model that could be used to unravel some of the complexities of the human immune system, including its responses to
    multiple types of pathogens," said Pranav Prabhala, a Technician at the
    Wyss Institute and second author of the paper.



    ========================================================================== Predicting vaccine efficacy on-a-chip Now that the scientists had a
    functional LF model that could initiate an immune response, they explored whether their LF Chip could be used to replicate and study the human
    immune system's response to vaccines.

    In the human body, vaccination induces special cells called dendritic
    cells to take up the injected pathogen and migrate to lymph nodes,
    where they present fragments of them on their surface. There, these antigen-presenting cells activate the B cells with the assistance of local
    T cells in the LF, causing the B cells to differentiate into plasma cells
    that produce antibodies against the pathogen. To replicate this process,
    the researchers added dendritic cells to LF Chips along with B and T
    cells from four separate human donors. They then inoculated the chips
    with a vaccine against the H5N1 strain of influenza along with an adjuvant called SWE that is known to boost immune responses to the vaccine.

    LF Chips that received the vaccine and the adjuvant produced significantly
    more plasma cells and anti-influenza antibodies than B and T cells grown
    in 2D cultures or LF Chips that received the vaccine but not the adjuvant.

    The team then repeated the experiment with cells from eight different
    donors, this time using the commercially available Fluzone?influenza
    vaccine, which protects against three different strains of the virus
    in humans. Once again, plasma cells and anti-influenza antibodies were
    present in significant numbers in the treated LF Chips. They also measured
    the levels of four cytokines in the vaccinated LF Chips that are known
    to be secreted by activated immune cells, and found that the levels of
    three of them (IFN-?, IL-10, and IL-2) were similar to those found in
    the serum of humans who had been vaccinated with Fluzone?.

    The Wyss researchers are now using their LF Chips to test various
    vaccines and adjuvants in collaboration with pharmaceutical companies
    and the Gates Foundation.

    "The flurry of vaccine development efforts sparked by the COVID-19
    pandemic were impressive for their speed, but the increased demand
    suddenly made traditional animal models scarce resources. The LF Chip
    offers a cheaper, faster, and more predictive model for studying human
    immune responses to both infections and vaccines, and we hope it will streamline and improve vaccine development against many diseases in
    the future," said corresponding author Donald Ingber, M.D., Ph.D.,
    who is the Founding Director of the Wyss Institute as well as the Judah
    Folkman Professor of Vascular Biology at Harvard Medical School (HMS)
    and Boston Children's Hospital, and Professor of Bioengineering at the
    Harvard John A. Paulson School of Engineering and Applied Sciences.

    Additional authors of the paper include Yunhao Zhai, Min Sun Kim, Aditya
    Patil, Danielle Curran, Jaclyn Long, Abidemi Junaid, and Tom Ferrante from
    the Wyss Institute; Bruce Bausk, Tal Gilboa, Limor Cohen, and David Walt
    from the Wyss Institute, Brigham and Women's Hospital, and HMS; and former
    Wyss Institute members Gautam Mahajan, Liangxia Xie, Roey Lazarovits,
    Adam Mansour, Sanjay Sharma, Oren Levy, and Rachelle Prantil-Baun.

    This research was supported by DARPA under Cooperative Agreement
    Number W911NF- 12-2-0036, the National Institutes of Health under
    grant UG3HL141797, the Bill and Melinda Gates Foundation, BARDA under
    contract 75A50121C00075, and the Wyss Institute for Biologically Inspired Engineering.


    ========================================================================== Story Source: Materials provided
    by Wyss_Institute_for_Biologically_Inspired_Engineering_at
    Harvard. Original written by Lindsay Brownell. Note: Content may be
    edited for style and length.


    ========================================================================== Journal Reference:
    1. Girija Goyal, Pranav Prabhala, Gautam Mahajan, Bruce Bausk,
    Tal Gilboa,
    Liangxia Xie, Yunhao Zhai, Roey Lazarovits, Adam Mansour,
    Min Sun Kim, Aditya Patil, Danielle Curran, Jaclyn M. Long,
    Sanjay Sharma, Abidemi Junaid, Limor Cohen, Thomas C. Ferrante,
    Oren Levy, Rachelle Prantil‐Baun, David R. Walt, Donald
    E. Ingber. Ectopic Lymphoid Follicle Formation and Human
    Seasonal Influenza Vaccination Responses Recapitulated in an
    Organ‐on‐a‐Chip. Advanced Science, 2022; 2103241
    DOI: 10.1002/advs.202103241 ==========================================================================

    Link to news story: https://www.sciencedaily.com/releases/2022/03/220315150120.htm

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