Dr.Jon Mochel, Director, Precision One Health, presents a seminar at UGA Institute of Bioinformatics

00:39:39
https://www.youtube.com/watch?v=y2Up_KMk6tw

Resumo

TLDRJohn, an expert in veterinary medicine and pharmacology, discusses his research on mathematical modeling to enhance the application of drugs in veterinary sciences. Educated in France and the Netherlands, with experience in the USA, he currently leads a One Health program at the University of Georgia. His talk explores how traditional human clinical drug trials are not feasible in veterinary practice due to smaller sample sizes and breed variations, necessitating alternative approaches. The research focuses on optimizing drug doses using models to bridge gaps between empirical practices and scientific evidence. He introduces a simulation tool used to personalize drug dosages in veterinary medicine, particularly for conditions like congestive heart failure in dogs. The concept of One Health is stressed, where insights from human and animal medicine are integrated to improve drug efficacy across species, aligning clinical practice with scientific research. John highlights the potential for translating animal health models into human medical advancements.

Conclusões

  • 🎓 John's education spans institutions in France and the Netherlands with a strong focus in veterinary medicine.
  • 🌟 He advocates for the simplification of complex scientific phenomena through straightforward models.
  • 🐾 The One Health approach: Integrating animal and human health for comprehensive disease understanding.
  • 💊 Computational models can overcome limitations of small sample sizes in veterinary drug trials.
  • 📊 Tool developed for optimizing cardiovascular drug doses in vet medicine, especially for heart diseases.
  • 🔍 Emphasis on biomarker correlation over traditional inhibitors for drug efficacy evaluation.
  • 🌍 Real-world practices often deviate from labeled drug recommendations, necessitating new models.
  • 🧩 Integration of data from clinical and preclinical studies to refine simulation accuracy.
  • 🔗 Cross-species insights: Translating veterinary drug application benefits into human medicine.
  • 🚀 Future research aims at conducting clinical trials to refine and validate dosage simulation tools.

Linha do tempo

  • 00:00:00 - 00:05:00

    The introduction presents the speaker's background in veterinary medicine and his roles, emphasizing his involvement in mathematical modeling to improve drug applications in veterinary medicine. His philosophy embraces simplicity in complex life processes. The limitations of drug trials in veterinary medicine are highlighted due to small sample sizes.

  • 00:05:00 - 00:10:00

    The speaker discusses the One Health program, which aims to bridge the gap between human and animal medicine by studying diseases common to both. He explains the concept of the renin-angiotensin system and its importance in maintaining life, highlighting a disconnect between recommended and practical drug doses.

  • 00:10:00 - 00:15:00

    This section delves into the complexity of the renin-angiotensin system (RAS), challenging the traditional biomarker approach. It argues that focusing on key biomarkers, such as angiotensin, is critical for understanding drug efficacy. The aim is to refine drug use in veterinary medicine based on real-world evidence.

  • 00:15:00 - 00:20:00

    It discusses the limitations of using small clinical trials and conventional statistics in veterinary medicine. The speaker advocates for advanced computational methods to improve clinical decision-making, highlighting a case study on optimizing ACE inhibitor doses in dogs with heart failure, bridging theory and practice.

  • 00:20:00 - 00:25:00

    The speaker explains a case study where mathematical modeling is used to evaluate the effects of ACE inhibitors on canine heart failure. He presents a detailed modeling approach that connects drug exposure with biological response, emphasizing the development of an online simulation tool for dose optimization.

  • 00:25:00 - 00:30:00

    The section covers the verification of the model's accuracy with real-world data and demonstrates its efficacy in optimizing drug doses. He emphasizes the differences seen between recommended and practically used doses, showing a significant benefit in using higher doses for heart disease in dogs.

  • 00:30:00 - 00:39:39

    Concluding the presentation, the speaker envisions future studies, focusing on making the tool more predictive by incorporating variables like dog breeds and disease stages. Potential collaboration with a drug company to enhance tool applicability in clinical settings is mentioned, alongside acknowledgements of contributors.

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Perguntas frequentes

  • What is the main focus of John's research presentation?

    John's presentation focuses on using mathematical modeling and pharmacology to optimize therapeutic drug use in veterinary medicine.

  • What educational background does John have?

    John got his Veterinary medical degree from the national veterinary school of Alford in Paris, France, collaborated with the College de France for his DVM, and completed a PhD at Leen University, Netherlands.

  • What is the One Health concept mentioned in the talk?

    The One Health concept integrates human, animal, and environmental health to understand disease dissemination across species and improve therapeutic drug development.

  • Why is there a need for different drug testing methods in veterinary medicine compared to human medicine?

    Veterinary medicine cannot conduct large-scale clinical trials like human medicine and has high variability in animal breeds, necessitating alternative drug testing methods.

  • What analogy does John use to describe complexity in his research?

    John uses the analogy of Picasso's bull, illustrating that complexity in life can be captured with simplicity, to explain his research philosophy.

  • What challenge does John's research aim to address?

    John's research aims to address the gap between clinical practice and labeled drug dosages, optimizing doses using mathematical models.

  • How does John's team plan to make the drug dosing tool more predictive?

    They plan to collect clinical data from dogs with cardiac issues and update the simulation model to improve its predictive accuracy for personalized medicine.

  • What is the current disconnect in drug dosage recommendations in veterinary medicine?

    The current dosage recommendations often differ from practicing veterinarians' observations, suggesting a potential benefit in higher doses than previously labeled.

  • How does computational modeling benefit veterinary drug development?

    By using mathematical models and simulations, computational modeling allows for optimization of drug dosages and understanding drug effects, compensating for small animal trial sizes and breed variability.

  • What future steps does John's team intend to take for their research?

    They intend to collaborate with drug companies to validate their simulation model with clinical trial data from diseased animals.

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Legendas
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Rolagem automática:
  • 00:00:00
    mle uh he's our speaker today he got his
  • 00:00:04
    Veterinary uh medical degree uh from the
  • 00:00:07
    national veterinary school of Alford
  • 00:00:10
    which is in Paris France and then went
  • 00:00:13
    on to DVM which was in collaboration
  • 00:00:15
    with the College de France then worked
  • 00:00:18
    on a PhD in Leen University which is in
  • 00:00:21
    the Netherlands and then he jumped the
  • 00:00:24
    pond uh to become a faculty member at
  • 00:00:28
    Iowa State University my old stomping
  • 00:00:30
    grounds and more recently uh he has
  • 00:00:33
    joined us here at ug in the department
  • 00:00:36
    of pathology in the College of vet
  • 00:00:39
    medicine and he's leading uh the program
  • 00:00:43
    in uh one Health uh here at UG and so
  • 00:00:47
    John uh welcome and please uh let us
  • 00:00:51
    know about your
  • 00:00:53
    work thank you so much Dr then for the
  • 00:00:56
    kind introduction and uh good morning
  • 00:00:59
    everyone it's great to be not
  • 00:01:02
    physically you guys but
  • 00:01:05
    virtually to present some of of our
  • 00:01:08
    research um in the field of compal
  • 00:01:11
    Sciences and comparative
  • 00:01:13
    medicine um so my job today you know is
  • 00:01:18
    and pharmacology uh can work together um
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    to create a tool that can be used for U
  • 00:01:25
    ped applications um not in human
  • 00:01:27
    medicine but in veter medicines so it's
  • 00:01:30
    a kind of a new and explored field those
  • 00:01:33
    far um but first um just a bit about my
  • 00:01:37
    research philosophy when it comes to
  • 00:01:40
    mathematical modeling um I'm pretty much
  • 00:01:43
    a fan of the keys Orit symbol approach
  • 00:01:47
    um and so this was the the cover of my
  • 00:01:49
    PhD work uh long time ago uh featuring
  • 00:01:53
    the uh the bull by Picasso uh which
  • 00:01:56
    illustrates the fact that complexity in
  • 00:01:58
    life can be Capt with just um six lines
  • 00:02:02
    right so I mean I'm a big fan of the uh
  • 00:02:05
    the the simplest way to basically
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    explain a very complex phenomenon um now
  • 00:02:10
    about the the science uh when you think
  • 00:02:13
    about drug research and development the
  • 00:02:16
    current Paradigm and I'm sure you know
  • 00:02:18
    that already is is well suited for human
  • 00:02:20
    clinical trials um you know when you
  • 00:02:23
    have the ability to enroll you know tens
  • 00:02:26
    of thousands to of patients and to
  • 00:02:30
    evaluate the effectiveness and safety of
  • 00:02:32
    new therapeutic drugs and um that is
  • 00:02:35
    something that we cannot afford um in VM
  • 00:02:38
    right so all trials include at most ands
  • 00:02:42
    of subjects typically less than that
  • 00:02:44
    maybe you know 50 to to 90 um and that's
  • 00:02:48
    also more complicated by the fact that
  • 00:02:50
    we have an extremely large viability in
  • 00:02:53
    the background and to differences in
  • 00:02:56
    breeds and so forth so we need to come
  • 00:02:58
    up with with alternative to train uh for
  • 00:03:02
    Innovation U before going into the
  • 00:03:04
    clinic um in veter
  • 00:03:07
    medicine and that's precisely one of the
  • 00:03:10
    objective of our lab um and this new
  • 00:03:12
    center for precision one Health at UG
  • 00:03:15
    and I'm sure you already know about the
  • 00:03:16
    concept of one Health in the in the
  • 00:03:18
    context of infectious disease and and
  • 00:03:21
    how interactions between the environment
  • 00:03:24
    the animals and humans can actually
  • 00:03:27
    facilitate dissemination of disease
  • 00:03:29
    between species and that's all
  • 00:03:31
    Foundation obviously but we want to also
  • 00:03:33
    expand on that concept to also include
  • 00:03:36
    any kind of disease that can be shared
  • 00:03:38
    between humans and animals such as
  • 00:03:41
    cancer uh kidney disease congestive
  • 00:03:44
    heart failure and so forth so we believe
  • 00:03:47
    that the information we can collect from
  • 00:03:49
    animal patients right not animal
  • 00:03:51
    subjects as as experimental test case um
  • 00:03:55
    can further our understanding of disease
  • 00:03:58
    pathogenesis and contribute to the
  • 00:04:00
    development of new therapeutic drugs for
  • 00:04:03
    humans and vice versa and and that's
  • 00:04:06
    what you know I think I I would like to
  • 00:04:08
    contribute um to your student body uh
  • 00:04:11
    providing an experience on how this uh
  • 00:04:14
    mathematical methods can help optimize
  • 00:04:18
    the use of therapeutic drugs in humans
  • 00:04:21
    and animal patients and so exporing them
  • 00:04:24
    you know to a broad and very large
  • 00:04:26
    variety of problems which are centered
  • 00:04:28
    around clinical applications um in the
  • 00:04:32
    end so um moving on to now our case
  • 00:04:35
    study for the day and so what I'm going
  • 00:04:38
    to try to do and to to actually you know
  • 00:04:41
    capture in the next um 30 minutes um is
  • 00:04:45
    is attempt to open the black box that
  • 00:04:47
    stands between um the
  • 00:04:51
    um the optimal dose of a cardiovascular
  • 00:04:55
    drug called an Ace inhibitor and which
  • 00:04:57
    is used for the treatment of congestive
  • 00:04:59
    heart failure and and and therapeutic
  • 00:05:01
    response and that's that's that's a
  • 00:05:03
    matter of you know of heavy debate uh in
  • 00:05:06
    in the vetmet community uh because the
  • 00:05:09
    current recommended dose of that drug is
  • 00:05:13
    25 milligram per kilogram once a day uh
  • 00:05:16
    but practitioners in practice use a much
  • 00:05:20
    higher dose uh which can be up to one
  • 00:05:23
    milligram per kilograms in total per day
  • 00:05:26
    and so there is kind of a disconnect
  • 00:05:28
    between what has been you know labeled
  • 00:05:30
    and uh used for uh registration 20 years
  • 00:05:34
    ago u based on some end points and some
  • 00:05:37
    preclinical studies and the reality of
  • 00:05:40
    what practicians do because they
  • 00:05:42
    actually observe a different kind of
  • 00:05:43
    response in their patient population so
  • 00:05:46
    um this job is this work is is is trying
  • 00:05:49
    to reconciliate clinical data with
  • 00:05:53
    mathematical modeling approach to kind
  • 00:05:55
    of you know optimize the use of these
  • 00:05:57
    drugs and their doses uh in dogs with
  • 00:06:01
    congestive heart failure uh because
  • 00:06:03
    similar to humans dogs also suffer from
  • 00:06:06
    cardiac disease um as you may already
  • 00:06:08
    know and so to to address this knowledge
  • 00:06:11
    Gap uh we need to revisit two paradigms
  • 00:06:15
    uh first the way we are approaching the
  • 00:06:17
    biology of what we call the the RAS or
  • 00:06:19
    reens aldosterone system which is this
  • 00:06:22
    background biological pathway uh which
  • 00:06:25
    is Target of this uh drug called an a
  • 00:06:29
    inhibitor and second the the methods we
  • 00:06:32
    use to quantify the effect of these
  • 00:06:34
    drugs or the ACE inhibitors on that
  • 00:06:37
    biological path which is called the the
  • 00:06:39
    rra or rensin system so we're going to
  • 00:06:42
    start quickly with the biology of this
  • 00:06:44
    of this pathway um and I don't know if
  • 00:06:47
    you're familiar with the rensin system
  • 00:06:49
    but it's kind of one of the the most
  • 00:06:50
    important um hormonal system to maintain
  • 00:06:53
    life um and to maintain blood pressure
  • 00:06:57
    um and it's actually a fairly
  • 00:06:59
    complicated
  • 00:07:00
    pathway which used to be you know known
  • 00:07:03
    to be centered around primarily two
  • 00:07:06
    biomarkers which we call angens in 2 and
  • 00:07:10
    aldosterone and and for years people
  • 00:07:13
    have simplified that pathway and that
  • 00:07:15
    Cascade with those two biomarkers and
  • 00:07:18
    the way we have been developing these
  • 00:07:20
    drugs called a Inhibitors is basically
  • 00:07:23
    to to Target that enzyme over there and
  • 00:07:26
    reduce the production of energ tens to
  • 00:07:28
    which we believe believe uh is related
  • 00:07:31
    to uh fibrosis in the art and in
  • 00:07:34
    different organs which leads to
  • 00:07:36
    congestive heart faure after many years
  • 00:07:38
    of being
  • 00:07:39
    overactivated but practically this you
  • 00:07:42
    know this simplistic approach is just
  • 00:07:44
    the tip of the isberg um so what we know
  • 00:07:47
    now is that there are multiple Pathways
  • 00:07:49
    of the of the rra um and we typically
  • 00:07:52
    you know use that classification between
  • 00:07:55
    the
  • 00:07:55
    conventional axis of the RAS which
  • 00:07:58
    revolves around ensine 2 here which we
  • 00:08:01
    discussed earlier and that is linked to
  • 00:08:04
    a series of negative effects such as
  • 00:08:07
    visoc constrictions um hypertrophy of
  • 00:08:10
    the heart fibrosis and so forth and then
  • 00:08:12
    an alternative pathway this time which
  • 00:08:15
    is cented around ensin 17 and one n
  • 00:08:19
    which
  • 00:08:20
    exert opposite effect to tinin 2 and so
  • 00:08:24
    they have actually beneficial effect
  • 00:08:26
    overall um including anti fibrosis
  • 00:08:29
    effect
  • 00:08:30
    anti-hypertrophic effect and
  • 00:08:32
    antioxidant effect and so when you try
  • 00:08:34
    to capture the effect of any drugs
  • 00:08:38
    interacting with that system what you
  • 00:08:40
    need to know and what you need to do is
  • 00:08:42
    to get a comprehensive overview of how
  • 00:08:45
    much is this negative arm of the RAS you
  • 00:08:48
    know activated so the ens two here and
  • 00:08:52
    how much is the positive arm of the rest
  • 00:08:54
    with ens in one n and S also stimulated
  • 00:08:58
    or inhibited will your medication so I'm
  • 00:09:01
    trying to use that analogy of you know
  • 00:09:03
    basically we have the the dark side
  • 00:09:05
    versus the the bright side of the rasp
  • 00:09:07
    when I explain that concept to to my
  • 00:09:10
    students so unfortunately um you know
  • 00:09:13
    most of the studies that were used 20
  • 00:09:15
    years ago to actually determine the dose
  • 00:09:17
    of these drugs in in veter medicine um
  • 00:09:20
    have been using that biomarker called
  • 00:09:23
    Ace activity as a proxy for clinical
  • 00:09:27
    efficacy and so Ace was just was
  • 00:09:29
    representing how much you know enzymatic
  • 00:09:32
    activity I had in my system and the goal
  • 00:09:35
    is was to basically you know shut it
  • 00:09:37
    down to almost zero to get to a
  • 00:09:39
    therapeutic clinical effect um and what
  • 00:09:42
    those Studies have shown is that you
  • 00:09:44
    know you don't need to go very high with
  • 00:09:46
    the dose of these drugs if you go to 25
  • 00:09:49
    milligram per kilogram once a day you
  • 00:09:51
    already kind of max out the effect on
  • 00:09:54
    that biomarker and that was kind of the
  • 00:09:56
    rational for you know this 25 Mig per
  • 00:09:59
    kilogram once the data was labeled uh
  • 00:10:02
    when registered in the EU and in the US
  • 00:10:05
    um as well actually unfortunately uh we
  • 00:10:09
    do know now that there is not a strict
  • 00:10:11
    correlation between the activity of the
  • 00:10:14
    enzyme and its product which is ens so
  • 00:10:18
    if I go back to this slide over there
  • 00:10:20
    you can see that Ace is responsible for
  • 00:10:23
    n to production but inhibiting that
  • 00:10:26
    enzyme over here does not lead to a
  • 00:10:29
    complete blockade and depletion of that
  • 00:10:32
    biomarker and so there is a disconnect
  • 00:10:34
    clinically between the level of Ace
  • 00:10:37
    inhibition you see in patients and the
  • 00:10:39
    amount of Anin 2 that they actually
  • 00:10:42
    produce um in their system and in fact
  • 00:10:45
    you know we know that up to half of
  • 00:10:48
    patients uh with complete depletion of
  • 00:10:52
    Ace activity still have pretty elevated
  • 00:10:55
    antin in two levels which we know are
  • 00:10:58
    you know prog IC for morbility and
  • 00:11:00
    mortality in in patients with kardiac
  • 00:11:03
    disease and so all of this that we need
  • 00:11:05
    to kind of shy away from you know walk
  • 00:11:08
    away from those old biomarkers Ace
  • 00:11:10
    inhibition to really capture the actual
  • 00:11:13
    therapeutic effect of these drugs and
  • 00:11:16
    what we know from Human studies is that
  • 00:11:17
    two biomarkers so antin in two here and
  • 00:11:21
    AD Doone particularly have been heavily
  • 00:11:24
    correlated with clinical outcomes in
  • 00:11:28
    patients with congestive heart failure
  • 00:11:31
    so we need to basically you know look at
  • 00:11:32
    those biomarkers more so than just
  • 00:11:34
    looking at a activity as a proxy for
  • 00:11:38
    clinical
  • 00:11:41
    activity now what I found to be very
  • 00:11:43
    interesting is that you know when you
  • 00:11:45
    look at the the information we get from
  • 00:11:48
    I'm going to create the real um the real
  • 00:11:50
    world evidence of these drugs is that
  • 00:11:54
    clinicians already use you know these a
  • 00:11:57
    Inhibitors at a much larger dose than
  • 00:12:00
    the one based on Ace activity alone as a
  • 00:12:04
    proxy ofin efficacy so as I was telling
  • 00:12:07
    you in my int you know practically the
  • 00:12:10
    current recommendations is to use that
  • 00:12:13
    drug or point5 milligram per kilogram
  • 00:12:16
    twice a day versus the 25 mix per
  • 00:12:20
    kilogram once a day there's a fourfold
  • 00:12:23
    difference between what was actually
  • 00:12:25
    used initially from labeling studies and
  • 00:12:28
    what clinicians you know recommend based
  • 00:12:30
    on the clinical expertise and so there
  • 00:12:32
    seems to be some kind of a of a you know
  • 00:12:36
    of a of a consensus between clinical
  • 00:12:38
    practice and what we know about the
  • 00:12:40
    biology of these drugs to maybe work on
  • 00:12:42
    you know an optimization uh
  • 00:12:45
    of of these drugs based on more you know
  • 00:12:48
    scientific evidence basically so uh know
  • 00:12:52
    that we actually know about the biology
  • 00:12:53
    of of the RAS um I'd like to discuss
  • 00:12:56
    some some
  • 00:12:57
    limitations uh of the method that we
  • 00:13:00
    actually use to quantify the effect of
  • 00:13:02
    of R Inhibitors especially in veteran
  • 00:13:06
    medicine so um maybe you remember this
  • 00:13:09
    this slide from the beginning um so in
  • 00:13:12
    practice you know what we what we do in
  • 00:13:14
    vetman is we have kind of small study
  • 00:13:17
    populations so we have clinical studies
  • 00:13:19
    of maybe 50 to 200 animals that we
  • 00:13:20
    actually use and to to verify the
  • 00:13:23
    efficacy and safety of drugs in the
  • 00:13:25
    clinic uh but we also have to face a lot
  • 00:13:29
    because of inherent background viability
  • 00:13:31
    that's really you know makes your life
  • 00:13:33
    more difficult to tease out a signal to
  • 00:13:36
    nose ratio so really finding an answer
  • 00:13:39
    in the clinic is often difficult
  • 00:13:42
    especially when you rely on you know
  • 00:13:44
    very conven statistics um because we
  • 00:13:47
    always very limited by the stample size
  • 00:13:49
    of our cohort and so you know trying to
  • 00:13:52
    make some generalization from a a c of
  • 00:13:55
    50 or 60 dogs of certain breed
  • 00:13:57
    characteristics to the entire population
  • 00:14:00
    of dogs is extremely as hardest um and
  • 00:14:03
    that's why you know we're trying to push
  • 00:14:05
    you know for the use of more um heavily
  • 00:14:08
    computational heavly methods such as MLS
  • 00:14:11
    and mathematical Ming and simulations to
  • 00:14:13
    kind of make a better job in know
  • 00:14:15
    inference to to make better decisions
  • 00:14:17
    when it comes to uh to doses um in those
  • 00:14:20
    dogs with congestive heart
  • 00:14:23
    failure
  • 00:14:24
    so that's probably you know one of the
  • 00:14:27
    uh the easiest way to to summarize this
  • 00:14:31
    information um and I wanted now to
  • 00:14:34
    really you know bring it on to this case
  • 00:14:36
    study about the optimization of of a
  • 00:14:38
    Inhibitors in dogs and with congestive
  • 00:14:41
    heart and then break you know through
  • 00:14:43
    that black box uh that stands between
  • 00:14:46
    the the dose of an a inhibitory and the
  • 00:14:49
    actual effect of that drug you know um
  • 00:14:52
    on the r system um and the only way to
  • 00:14:55
    do this is to look at the exposure right
  • 00:14:57
    so basically what what we wanted to do
  • 00:14:59
    with that study is one uh characterize
  • 00:15:03
    the exposure response relationship of
  • 00:15:05
    ACE inhibitors on biomarkers which we
  • 00:15:09
    know are relevant to congestive heart
  • 00:15:11
    failure in dogs which are N2 um N17 and
  • 00:15:15
    N one9 particularly and then build a
  • 00:15:19
    simulator that basically would help us
  • 00:15:21
    to optimize the dose of these drugs
  • 00:15:24
    using different whatif
  • 00:15:27
    scenarios so I I won't spend too much
  • 00:15:30
    time on this slide which is pretty
  • 00:15:31
    crowded already but just to give you a
  • 00:15:33
    bit of a of an overview so what we did
  • 00:15:35
    is we actually connected a study um in
  • 00:15:38
    healthy dogs um and we actually have
  • 00:15:40
    three groups receiving different doses
  • 00:15:43
    of Naas Inhibitors uh using a partial
  • 00:15:46
    crossover design and so we use doses
  • 00:15:48
    from 0.1 to five mix pii twice a day 2.5
  • 00:15:53
    mix pck twice a day uh once a day sorry
  • 00:15:55
    as well in those dogs and then we sample
  • 00:15:58
    them over time for looking at those
  • 00:16:00
    biomarkers and the
  • 00:16:05
    concentration of the ace inhibitor in
  • 00:16:08
    the blood of these dogs and the all the
  • 00:16:11
    overall goal of this exercise was to
  • 00:16:13
    correlate drug exposure over time with
  • 00:16:16
    the pharmacodynamic response we observed
  • 00:16:19
    under different biomarkers of the r and
  • 00:16:21
    then build a mathematical model related
  • 00:16:24
    dally the drug concentration to the drug
  • 00:16:28
    efficacy on those biomarkers to build
  • 00:16:31
    this online simulator so on top of this
  • 00:16:34
    biomarkers we also collected you know
  • 00:16:36
    different measures such as blood
  • 00:16:37
    pressure and some Eco of the heart to
  • 00:16:39
    check for the you know functional uh
  • 00:16:41
    changes over time as well but really the
  • 00:16:43
    the the majority of the work was
  • 00:16:45
    focusing on collecting blood for
  • 00:16:48
    characterizing the PKS or the exposure
  • 00:16:50
    of the drug and the P so the effect uh
  • 00:16:55
    of these drugs
  • 00:17:01
    on the
  • 00:17:02
    renon systems um of those the um the
  • 00:17:06
    diagram of the mathematical model the
  • 00:17:07
    mechanistic model we built and
  • 00:17:11
    to of baz which is the name of this drug
  • 00:17:14
    where on the different
  • 00:17:16
    biomarkers of the RAS so very very
  • 00:17:20
    briefly again I don't want to go into
  • 00:17:22
    too much detail here but this is this
  • 00:17:25
    portion here that I'm highlighting over
  • 00:17:28
    here is is the kinetic model that we
  • 00:17:30
    have developed it's basically based on
  • 00:17:33
    The Binding model of
  • 00:17:36
    the
  • 00:17:39
    enzy to its drug which is to basically
  • 00:17:42
    you know modify the mment and kinetics
  • 00:17:46
    uh of the virus than anen which are
  • 00:17:49
    related to the production of gensin one
  • 00:17:53
    and two you know in in the blood and
  • 00:17:56
    then we had a very similar model for the
  • 00:17:58
    tissue component of that system because
  • 00:18:00
    the RAS is actually found both in the
  • 00:18:03
    systemic circulation and in different
  • 00:18:06
    tissue compartments so we had one model
  • 00:18:09
    for the blood and one model for the
  • 00:18:11
    tissue in equilibrium and then we use
  • 00:18:13
    different OD systems to basically model
  • 00:18:16
    the PK and PD of Bazil on those
  • 00:18:20
    different
  • 00:18:21
    biomarkers so this next uh set of slides
  • 00:18:25
    present the the goodness of fit uh of
  • 00:18:28
    the model uh based on the observation
  • 00:18:31
    versus prediction plot so as you can see
  • 00:18:33
    we have here the goodness of f for the
  • 00:18:35
    PK of the drug so the kinetic of the
  • 00:18:37
    drug for bazat right in the plasma of
  • 00:18:40
    those drugs and then we had the same
  • 00:18:42
    things for the virus biomarkers so which
  • 00:18:43
    basically again translate the effect of
  • 00:18:46
    that drug for ensin one 2 17 and then
  • 00:18:51
    other
  • 00:18:52
    ensin and as you can see uh from that
  • 00:18:55
    graph you know we had a a very good
  • 00:18:57
    agreement between the model based
  • 00:18:59
    predictions and the actual observations
  • 00:19:01
    over that populations of dogs so we get
  • 00:19:04
    some you know consistency across the
  • 00:19:06
    different biomarkers that the model was
  • 00:19:08
    able to capture most of the signal uh in
  • 00:19:11
    in this
  • 00:19:12
    do now looking at some individual fit
  • 00:19:15
    this time again you know what we can see
  • 00:19:16
    across the various biomarkers that we
  • 00:19:18
    have U we have sampled um is that we
  • 00:19:21
    were able to overall nicely captured
  • 00:19:23
    individual Dynamic of the of the PK and
  • 00:19:26
    on the and of the response um for these
  • 00:19:30
    different um you know dogs as well so
  • 00:19:34
    again we checking that box we we are
  • 00:19:36
    pretty happy with the performance of
  • 00:19:39
    theel and then you know once we had
  • 00:19:42
    confidence about the ability of that
  • 00:19:44
    model to really cap to the pnpd of this
  • 00:19:47
    ACE inhibitors on the virus and 10 since
  • 00:19:50
    we knew we were actually able to
  • 00:19:53
    build a simulation tool to really look
  • 00:19:56
    at the relationship between those
  • 00:19:59
    exposure and response and then optimize
  • 00:20:01
    uh the dose of ANH inhibitor that we can
  • 00:20:04
    actually use uh in a patient population
  • 00:20:07
    uh so that's the the FR part of the
  • 00:20:08
    exercise the simulation step and so now
  • 00:20:11
    if you actually um um uh take a a print
  • 00:20:14
    SCP of that of that QR code here uh it
  • 00:20:17
    brings you to an online simulator which
  • 00:20:20
    I'm going to open in just a in just a
  • 00:20:22
    second so then we have the exact same
  • 00:20:25
    thing Al
  • 00:20:27
    together so
  • 00:20:44
    all right I'm going to reshare my screen
  • 00:20:47
    again all right so hopefully this will
  • 00:20:51
    work because the network is not great
  • 00:20:53
    but you should be able
  • 00:20:55
    to to see what I'm doing so let's
  • 00:21:01
    see from here all right all right so
  • 00:21:05
    hopefully you you do see uh my brother
  • 00:21:09
    uh and so if you actually look at here
  • 00:21:12
    you have different tabs and one of these
  • 00:21:14
    tabs is the dosage comparison um and so
  • 00:21:17
    if you know look at here you can compare
  • 00:21:19
    up to four different dozing schedule um
  • 00:21:23
    I'm going to select maybe just two so
  • 00:21:26
    that's here the first one be the actual
  • 00:21:29
    currently uh label dose of this stroke
  • 00:21:32
    which is25 mix per cake for just once a
  • 00:21:36
    day um and I'm going to give to that
  • 00:21:39
    virtual dog
  • 00:21:45
    s and then the second one is the most
  • 00:21:48
    twice a day this time um and again I'm
  • 00:21:50
    going to give it this time for seven
  • 00:21:51
    days so 14 in total because we give the
  • 00:21:53
    drug in that that case twice a day and
  • 00:21:58
    then you just click on run comparison
  • 00:22:00
    over here um it's going to run those
  • 00:22:02
    simulations in the background um and if
  • 00:22:04
    we're lucky and the internet Lowes we're
  • 00:22:07
    going to see now the results of those
  • 00:22:10
    simulations uh so that what you see here
  • 00:22:15
    so the yellow um plots are for the the
  • 00:22:18
    most extreme dose like the high dose of
  • 00:22:20
    0.5 makes per kick twice a day and the
  • 00:22:23
    blue is a result of those simulations
  • 00:22:24
    for the lower dose of 25 mix per kick
  • 00:22:28
    one once a day here you actually have
  • 00:22:30
    the the PK of the drug which is the
  • 00:22:32
    concentration time course for the ACE
  • 00:22:35
    inhibitors and then for the different
  • 00:22:37
    panels over there you see the Dynamics
  • 00:22:39
    of the response for the various and
  • 00:22:41
    tensins that belong to the rensin system
  • 00:22:47
    so arm and the alternative arm T
  • 00:22:51
    response because we also had a PLO model
  • 00:22:54
    embedded into our simulator right so
  • 00:22:56
    what you can actually see here is that
  • 00:22:58
    now you have a different um um tabulated
  • 00:23:02
    numbers and so we have we can calculate
  • 00:23:05
    the area the curve at different times
  • 00:23:08
    and then ask you know the the program to
  • 00:23:11
    calculate for us what the values does
  • 00:23:14
    the are of the curve versus the PLO for
  • 00:23:17
    the two we have been investigated and
  • 00:23:21
    together with the
  • 00:23:23
    N9 and tradition interval from those
  • 00:23:26
    simulations so and you can do that for
  • 00:23:28
    all the biomarkers and if you look for
  • 00:23:30
    instance for ensine 2 which we know is
  • 00:23:32
    I'm going to call it the bad guy you
  • 00:23:34
    know which is related to the negative
  • 00:23:36
    effect of the RAS we had about a 30%
  • 00:23:40
    difference between the um the low dose
  • 00:23:43
    and the high do of the ACE inhibitors
  • 00:23:47
    now if I look at and 17 which is the the
  • 00:23:50
    good arm um of the RAS uh we had about a
  • 00:23:54
    50 to 55% difference between the low do
  • 00:23:58
    do and the high do so those simulations
  • 00:24:00
    are overall pretty consistent across the
  • 00:24:03
    different biomarkers and it seems that
  • 00:24:05
    you know if you actually go from the
  • 00:24:07
    lados to the hios you do have a
  • 00:24:10
    significant benefit in terms of you know
  • 00:24:13
    inhibiting the the the the arm of the of
  • 00:24:17
    the RAS which is ENT two and stimulating
  • 00:24:20
    this time the positive arm of the r
  • 00:24:22
    which is ENT 17 so that's exactly what
  • 00:24:25
    you want to see you want to reduce the
  • 00:24:27
    negative arm and stimulate the positive
  • 00:24:30
    arm and overall you actually manage to
  • 00:24:34
    do this much more effectively by using
  • 00:24:37
    the higher dose of P five Mix B kick
  • 00:24:40
    twice a day um in those dogs so now I'm
  • 00:24:43
    going to go back to my PowerPoint so I'm
  • 00:24:46
    going to stop share here and I'm going
  • 00:24:48
    to go back over
  • 00:24:51
    here and I'm going to do a share
  • 00:24:56
    again all right
  • 00:25:00
    so hopefully you do see my screen now
  • 00:25:03
    again um so as I was we have
  • 00:25:07
    three different
  • 00:25:10
    panel for that stimulators uh one
  • 00:25:15
    specifies the the drug do schedule you
  • 00:25:19
    play with how many you know dog can be
  • 00:25:21
    up to actually downloading the figures
  • 00:25:23
    from those simulations if you want to
  • 00:25:24
    keep those for your records um and as I
  • 00:25:26
    was telling you we calculate the end of
  • 00:25:28
    the curve uh and Weare those between
  • 00:25:33
    between does and and
  • 00:25:35
    Placebo uh so just to give you a bit of
  • 00:25:38
    a of a summary a Next Step from this
  • 00:25:40
    work um so what we actually saw was that
  • 00:25:43
    the most Rous response uh on the ens 2
  • 00:25:47
    which is again the the negative armor of
  • 00:25:49
    the RAS was really seen with the 05 mix
  • 00:25:52
    the twice the dead
  • 00:25:53
    doses um
  • 00:25:57
    and you know I did not run
  • 00:26:00
    this here um for the sake of time but if
  • 00:26:04
    you were doing the exact same for the 25
  • 00:26:06
    mix Pi but twice today
  • 00:26:15
    is you had actually I'm going to call
  • 00:26:18
    the middle dose so the 0 25 higher dose
  • 00:26:20
    when it comes to reducing ense into
  • 00:26:22
    concentrations in those in those virtual
  • 00:26:23
    patients um for N17 uh same thing uh the
  • 00:26:26
    most response was also seen with the
  • 00:26:28
    high of .5 mix thei twice today and as
  • 00:26:32
    we did see for instance into if we had
  • 00:26:36
    run the simulations for the 0 25 mix Pi
  • 00:26:39
    twice a day we also had about a 25 to
  • 00:26:41
    30% difference compared to the higher
  • 00:26:44
    dose also um a fairly close runner up
  • 00:26:47
    versus the high
  • 00:26:49
    do so basically you know based on those
  • 00:26:51
    simulations the the the 25 MI
  • 00:27:04
    produc some Conant and
  • 00:27:08
    more results and they were overall
  • 00:27:10
    superior to the current label ones today
  • 00:27:14
    so
  • 00:27:28
    uh simulations would
  • 00:27:37
    actually with a clinical practice that
  • 00:27:42
    you know basically phys recommend to use
  • 00:27:45
    these drugs
  • 00:27:47
    and as well but the are
  • 00:27:51
    B from in healthy dogs uh
  • 00:28:19
    all right so John was joining us from
  • 00:28:21
    Europe uh he was kind enough to be
  • 00:28:25
    joining us from a long way away uh so
  • 00:28:28
    we'll see if we can get him
  • 00:28:31
    back oh I I i'
  • 00:28:36
    be
  • 00:28:39
    hello oh I think you're there yep you're
  • 00:28:45
    back do do you hear me we
  • 00:28:50
    can all right super I'm sorry about this
  • 00:28:53
    uh I don't know when it stopped was it
  • 00:28:56
    at the conclusion level or
  • 00:29:00
    did you do you did you hear the
  • 00:29:02
    conclusions or should I repeat that if
  • 00:29:05
    you could repeat the conclusions that'd
  • 00:29:06
    be
  • 00:29:08
    great
  • 00:29:10
    yes okay absolutely I'm sorry about this
  • 00:29:13
    I knew that there going to be a a
  • 00:29:15
    problem with uh using the conference
  • 00:29:18
    center network but U you did pretty good
  • 00:29:21
    there were only very few times when it
  • 00:29:23
    dropped
  • 00:29:26
    out okay okay I guess I I kind of
  • 00:29:30
    uh I broke the system with the
  • 00:29:32
    simulations it was just too
  • 00:29:37
    much so no I was actually saying um in
  • 00:29:41
    conclusion that you know those
  • 00:29:42
    recommending practice for the canine
  • 00:29:45
    patients uh which is the at least in one
  • 00:29:48
    of the very first example that you know
  • 00:29:50
    we can actually reconciliate empirism
  • 00:29:53
    with um background um uh simulation
  • 00:30:00
    um
  • 00:30:02
    but it's these are been
  • 00:30:07
    bed only on healthy animals and so you
  • 00:30:11
    know it's actually a bit of of a risk on
  • 00:30:13
    data from healthy animals through things
  • 00:30:16
    in healthy
  • 00:30:17
    dogs is data coming from Clinical
  • 00:30:20
    patients so measuring the r of those
  • 00:30:23
    dogs you know in the clinic and then
  • 00:30:25
    fitting the simulator with actual data
  • 00:30:29
    from Clinical patients with congestive
  • 00:30:31
    heart failure is the next step to make
  • 00:30:33
    that tool more predictive and you know
  • 00:30:35
    we can also maybe make it a bit more
  • 00:30:37
    fine-tune to include some coite such as
  • 00:30:40
    breed or stage of disease to make that
  • 00:30:42
    really more of a tool for personalized
  • 00:30:44
    medicine applications and be more
  • 00:30:46
    specific to individual patient this time
  • 00:30:49
    and so what we're trying to do right now
  • 00:30:50
    is to to speak with the company who
  • 00:30:53
    actually sells that drug and convince
  • 00:30:56
    them to use those data to the
  • 00:30:58
    prospective study with different doses
  • 00:31:00
    of an a inhibitor and then to get data
  • 00:31:04
    from dogs with kajak disease blood uh
  • 00:31:07
    take blood from them and then feed them
  • 00:31:09
    all make it more productive moving
  • 00:31:10
    forward so that's kind of a what I'm
  • 00:31:12
    working right now with with a drug
  • 00:31:13
    company that sells the drug in the first
  • 00:31:15
    place um and last thing uh obviously you
  • 00:31:19
    know this is not uh only my work um it's
  • 00:31:22
    been basically the the the work of one
  • 00:31:24
    of my um previous po doog Ben um who
  • 00:31:28
    since then has moved to Industry so you
  • 00:31:31
    Tech me if you join
  • 00:31:34
    the you know the dark side of the of the
  • 00:31:38
    force I don't know but actually did a he
  • 00:31:40
    did a fantastic job over three years to
  • 00:31:42
    get that project to conclusion so um
  • 00:31:45
    with that you know I'd like to thank you
  • 00:31:47
    again for this you know um opportunity
  • 00:31:49
    to present this work um on using
  • 00:31:51
    mathematics um in for treating a problem
  • 00:31:53
    in dogs with congestive heart failure um
  • 00:31:56
    it's been a it's been a very fun journey
  • 00:31:58
    and so what I'm trying to do with my
  • 00:32:01
    with my students in the lab is really to
  • 00:32:03
    expose them to a lot of different cases
  • 00:32:06
    uh which are very very practical and
  • 00:32:08
    clinically oriented and then basically
  • 00:32:10
    Intrigue them as to how mathematics can
  • 00:32:12
    Bally be the bridge between science and
  • 00:32:15
    Clinics um and we are lucky that if
  • 00:32:17
    we're lucky but we are fortunate that
  • 00:32:20
    most of this disease also exist in
  • 00:32:22
    humans and so we not only want to use
  • 00:32:25
    those data to support you know uh
  • 00:32:27
    science for dogs but also to support the
  • 00:32:29
    way we using these
  • 00:32:33
    drugs human patients as well so we want
  • 00:32:35
    to make it a one Health exercise also
  • 00:32:38
    ultimately um so with that I'd be happy
  • 00:32:41
    to take any question I would like to
  • 00:32:42
    thank you for your
  • 00:32:45
    attention awesome thank you very much if
  • 00:32:48
    people have questions go ahead
  • 00:33:07
    hey John um you know me I think uh for
  • 00:33:10
    this audience uh you touched on this a
  • 00:33:12
    little bit briefly
  • 00:33:14
    um um but you talked a little bit about
  • 00:33:17
    kind of machine learning and biomarkers
  • 00:33:19
    um but also like deterministic modeling
  • 00:33:21
    like OD type modeling I think um
  • 00:33:23
    especially for this audience the kind of
  • 00:33:26
    General connections between these two
  • 00:33:28
    especially for precision one Health
  • 00:33:30
    might be um might be helpful you know
  • 00:33:32
    because I think a lot of people in the
  • 00:33:34
    audience they kind of do um you know
  • 00:33:37
    they work with various omix type data um
  • 00:33:40
    or they do um some sort of first
  • 00:33:43
    principal space modeling but I feel like
  • 00:33:45
    it's often not both or at least in those
  • 00:33:47
    types of projects um often don't overlap
  • 00:33:51
    so it's just wondering if you could like
  • 00:33:52
    talk about that dichotomy and how your
  • 00:33:55
    guys work um kind of bridges that
  • 00:33:59
    yeah absolutely so so just give bit of a
  • 00:34:01
    background I mean when you develop a
  • 00:34:03
    drug um for for Animals there is not any
  • 00:34:06
    requirement from the F that you collect
  • 00:34:08
    any um data for u p characterization so
  • 00:34:12
    people don't really look about the
  • 00:34:14
    exposure response of drugs and to
  • 00:34:17
    get a drug approved on the market in
  • 00:34:24
    the so you know we actually are um at
  • 00:34:27
    the level of quantitive science we have
  • 00:34:29
    on those studies is is fairly fairly
  • 00:34:31
    small and so what we're trying to do you
  • 00:34:33
    know with with our with our approaches
  • 00:34:35
    say okay we we're going to take what is
  • 00:34:37
    the best of
  • 00:34:39
    Theo on The Human Side um and try to
  • 00:34:42
    flip a bit the Paradigm and so um
  • 00:34:45
    focusing on on common in dogs and humans
  • 00:34:48
    such as cancer for instance we can we
  • 00:34:51
    collect a lot of biomarker informations
  • 00:34:53
    both from preclinical dogs clinical dogs
  • 00:34:56
    and individual as well um and we use a
  • 00:34:59
    variety of approach as even was alled to
  • 00:35:01
    such as omx or um also obviously
  • 00:35:05
    biomarker information and to try to
  • 00:35:08
    tease out you know what is the
  • 00:35:10
    relationship between the drug
  • 00:35:11
    concentration we we actually use um and
  • 00:35:15
    the effect we see with a big question
  • 00:35:17
    which is about extrapolation and scaling
  • 00:35:19
    um so what we actually see you know in a
  • 00:35:21
    dish uh or in a dog uh does not mean
  • 00:35:25
    that this is what you expect to see in
  • 00:35:27
    an actual human patient for instance so
  • 00:35:29
    you know when I see an ice killing of a
  • 00:35:32
    tumor uh coming from a dogs who is maybe
  • 00:35:35
    osteos saroma and I I would like to ex
  • 00:35:37
    that finding from dogs to humans then
  • 00:35:40
    the questions arise as to how do you
  • 00:35:41
    scale this up and so we also do a a fair
  • 00:35:44
    amount of u between species
  • 00:35:46
    extrapolation modeling uh to come up
  • 00:35:49
    with ways to um to make sense of this
  • 00:35:52
    data in the context of treating human
  • 00:35:55
    patient and so olab is kind of a uh I'm
  • 00:35:58
    going to create a mix bag um that you
  • 00:36:00
    know combines uh inv vitous systems um
  • 00:36:04
    invo studies in in healthy dogs and in
  • 00:36:07
    also disease dogs from the teaching
  • 00:36:09
    hospital that we have here in vetmet and
  • 00:36:12
    then using mathematics to kind of
  • 00:36:14
    extrapolate those findings from those
  • 00:36:15
    different sit situations to what we do
  • 00:36:18
    expect to see uh in a patient that has
  • 00:36:22
    the same disease you know like a human
  • 00:36:23
    patient in that case so it's kind of a
  • 00:36:25
    an exercise of jumping across as cell
  • 00:36:29
    systems uh animal models and then
  • 00:36:32
    species
  • 00:36:33
    ultimately yeah and I think just to
  • 00:36:35
    editorialize a little bit a lot of us
  • 00:36:37
    and I we cover different um model
  • 00:36:39
    systems model organisms I think that
  • 00:36:41
    cross organism stuff that you guys do in
  • 00:36:42
    the vet school could be an asset for
  • 00:36:45
    helping us all collaborate a little bit
  • 00:36:46
    more so anyway thanks absolutely
  • 00:36:49
    absolutely absolutely big
  • 00:36:54
    time are you able to see the chat John
  • 00:37:03
    yes all
  • 00:37:06
    right okay can you write examples
  • 00:37:11
    oh yes absolutely uh so I can give you a
  • 00:37:15
    a very concrete example so right now we
  • 00:37:17
    are working on um stem cell derived
  • 00:37:20
    organoids uh which are like you know Min
  • 00:37:22
    organs in a dish um and so we collect
  • 00:37:25
    basically tissue samples from the f with
  • 00:37:28
    different diseases um and then we grow
  • 00:37:30
    them you know we grow either the tumors
  • 00:37:32
    or the organs in a dish and we do a lot
  • 00:37:35
    of things such are in sequencing to
  • 00:37:38
    dissect you know the the pathophysiology
  • 00:37:41
    of a disease
  • 00:37:43
    or look at the effect um of a drug using
  • 00:37:47
    different mix approach um and right now
  • 00:37:49
    I work with a student which you helps us
  • 00:37:52
    with that pipeline to to analyze all of
  • 00:37:53
    the data coming from o sequencing and
  • 00:37:56
    then understand a you know what is the
  • 00:37:59
    pathways involved in this development
  • 00:38:02
    and B you know what is the effect and
  • 00:38:05
    what is the efficacy of different drugs
  • 00:38:06
    we're trying to use to uh to modulate
  • 00:38:09
    those disease in the first place um and
  • 00:38:11
    obviously you know in that exercise
  • 00:38:13
    we're trying to also look at um um
  • 00:38:16
    similar pathway between dogs and humans
  • 00:38:19
    and then hit on different targets that
  • 00:38:21
    we can use for drug development on both
  • 00:38:23
    ends so that's one example um the second
  • 00:38:26
    one I can give you is that we're working
  • 00:38:28
    also on on a program which is about
  • 00:38:29
    Cushing the
  • 00:39:08
    so we caught all the first one we're
  • 00:39:10
    missing the second one here I'm not sure
  • 00:39:12
    if John can hear me
  • 00:39:28
    I think he's gone again
Etiquetas
  • Veterinary Medicine
  • Pharmacology
  • Mathematical Modeling
  • One Health
  • Drug Development
  • Cardiac Disease
  • Clinical Trials
  • Animal Health
  • Therapeutic Drugs
  • Veterinary Pharmacology