University Medical Center, Inc. D/B/A James Graham Brown Cancer Center v. Reagan Brooke Shwab ( 2021 )


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  •                                                 RENDERED: AUGUST 26, 2021
    TO BE PUBLISHED
    Supreme Court of Kentucky
    2019-SC-0641-DG
    UNIVERSITY MEDICAL CENTER, INC.                                     APPELLANTS
    D/B/A JAMES GRAHAM BROWN
    CANCER CENTER; CRAIG L.
    SILVERMAN, M.D.; ROGER H.
    HERZIG, M.D.; AND UNIVERSITY
    MEDICAL CENTER, INC. D/B/A
    UNIVERSITY OF LOUISVILLE
    HOSPITAL
    ON REVIEW FROM COURT OF APPEALS
    V.                        NO. 2018-CA-1188
    JEFFERSON CIRCUIT COURT NO. 10-CI-006202
    REAGAN BROOKE SHWAB AND                                              APPELLEES
    HUGH MCNEILLY SHWAB, IV
    OPINION OF THE COURT BY JUSTICE HUGHES
    REVERSING AND REMANDING
    Reagan Brooke Shwab (Brooke) was diagnosed with a kidney disease
    which became severe in 2007, necessitating a kidney transplant. Interested in
    avoiding the need for lifetime immunosuppressant drugs following the
    transplant, Brooke consented to participate in a Phase I clinical trial that had
    as its goal participants achieving tolerance of a transplanted kidney and
    avoiding a continuing regimen of immunosuppressant drugs. Shortly after
    participating in the clinical trial, Brooke developed myelodysplastic syndrome
    (MDS), a rare form of blood cancer.
    Brooke and her husband filed suit against the clinical trial’s medical
    providers alleging that her consent to the medical treatment involved in the
    trial was invalid pursuant to Kentucky Revised Statute (KRS) 304.40-320, the
    statute that provides the framework for determining when informed consent
    has been properly given in an action involving medical care. After eight years
    of discovery, the trial court found that the informed consent in this case
    complied with Kentucky statutory authority and federal regulations and
    granted summary judgment to the medical defendants. The Court of Appeals
    reversed, holding that the Shwabs presented enough evidence to potentially
    convince a jury that the medical defendants did not give them enough
    information to reasonably understand the clinical trial or the potential risks.
    After careful review, we reverse the Court of Appeals and reinstate the trial
    court’s judgment.
    FACTS AND PROCEDURAL HISTORY
    In 1996 Reagan Brooke Shwab was diagnosed with IgA nephropathy, a
    kidney disease in which antibodies build up and damage kidney tissues.1 In
    2007 the disease became so severe that she began dialysis. Shortly after
    beginning dialysis her kidneys began failing and she needed a transplant.
    Brooke’s nephrologist, Dr. Sanford Reikes, referred her to Dr. Kadiyala
    Ravindra and the organ transplant team at Jewish Hospital in Louisville,
    1 IgA nephropathy (Berger’s disease), MAYO CLINIC (May 17, 2019),
    https://www.mayoclinic.org/diseases-conditions/iga-nephropathy/symptoms-
    causes/syc-20352268.
    2
    Kentucky. The transplant team determined that Brooke was a transplant
    candidate and her husband, Hugh “Mack” Shwab, was an eligible donor.
    The Shwabs, both college-educated individuals, met with Dr. Ravindra
    on January 24, 2008 to discuss the transplant process and her need to take
    immunosuppressant drugs after the transplant. They also discussed possible
    complications related to the immunosuppressant drugs. During this meeting
    the Shwabs asked about a clinical trial involving bone marrow transfusion that
    Mack’s mother had heard about on the radio. Dr. Ravindra, the trial’s
    principal investigator and transplant specialist, explained the trial and its past
    results.
    In 2003 the Institute of Cellular Therapeutics (ICT) and the James
    Graham Brown Cancer Center at the University of Louisville partnered with the
    Northwestern School of Medicine to conduct a Phase I clinical trial involving
    kidney transplants.2 The trial’s ultimate goal was to allow a subject’s body to
    develop “tolerance” to the transplanted kidney and thereby avoid the need for
    long-term anti-rejection drug therapy. The clinical trial used a combination of
    a stem cell transplant and kidney transplantation from the same donor, along
    with sequential chemotherapy and total body irradiation.3 The trial began in
    2 The study was called “Induction of Donor Specific Tolerance in Recipients of
    Live Donor Kidney Allografts by Donor Stem Cell Infusion” (hereafter referred to as
    Phase I clinical trial or clinical trial).
    3 Total body irradiation, as explained in the materials provided to Brooke, is
    radiation therapy involving the use of high energy x-rays directed to the entire body.
    The purpose of total body irradiation is to kill cancer or abnormal cells and suppress
    the immune system before transplantation with healthy bone marrow.
    3
    2003 and was sponsored by Dr. Suzanne Ildstad, a professor of transplantation
    and surgery at the University of Louisville who focused her research on ways to
    induce tolerance in transplant patients.
    Clinical trials range from Phases I through IV.4 A Phase I trial is an
    initial safety trial on a new medicine or treatment, usually done with a small
    group of people to begin identifying unknown side effects.5 Phase I trials are
    focused on establishing tolerability, i.e., whether the patient tolerates the
    medication or procedure, primarily looking for indices of safety.6 Because a
    Phase I clinical trial’s process and procedures are previously untested in
    humans, toxicity is unknown, and safety cannot be guaranteed.7
    Several meetings occurred between the Shwabs and various medical
    providers regarding the clinical trial. After their initial discussions about the
    clinical trial Dr. Ravindra introduced the Shwabs to Elizabeth Reed, the trial’s
    clinical nurse manager. Reed spoke with the Shwabs for approximately fifteen
    to twenty minutes and explained the nature of a Phase I trial and the trial
    protocol.
    The protocol for the trial proceeded as follows: the patient would receive
    chemotherapy for three days to suppress the immune system; the following
    4 There are five phases of clinical trials: Early Phase 1 (formerly known as Phase
    0), Phase I, Phase II, Phase III and Phase IV. U.S. National Library of Medicine, Learn
    About Clinical Studies, https://clinicaltrials.gov/ct2/about-studies/learn (last updated
    Mar. 2019).
    5   Id.
    6   Id.
    7   Id.
    4
    day, the patient would undergo total body irradiation; the day after the
    radiation, the patient would receive an infusion of stem cells from the kidney
    donor; and one to two months later the patient would receive the kidney
    transplant.8 The goal of the trial was to make the participant’s body more
    receptive to the donated kidney and negate the need for anti-rejection and
    immunosuppressant drugs after the transplant.
    The Food and Drug Administration (FDA), tasked with ensuring the
    protection of the rights, safety and welfare of human subjects who participate
    in clinical trials, reviewed the clinical trial protocol and consent form. 21
    United States Code (U.S.C.) Chapter 9. Because the clinical trial was
    regulated, in part, by the FDA, the clinical trial had to satisfy federal
    regulations governing the protection of human subjects. 21 Code of Federal
    Regulations (C.F.R.) Part 50. The clinical trial was funded in part by the
    United States Department of Defense, which also reviewed the protocol and
    informed consent form. In addition, the Department of Defense requires the
    use of a Data Safety Monitoring Board which consists of a group of
    independent scientists who monitor the safety and integrity of a clinical trial.9
    8   Brooke was one of the first participants to undergo this specific protocol. The
    trial originally began in 2003 and involved simultaneous conditioning, bone marrow
    transplant, and kidney transplant. Over four years approximately twelve participants
    underwent the protocol, but it was relatively unsuccessful. Immediately prior to
    Brooke’s participation, the protocol was changed to a sequential approach. The trial’s
    investigators believed there would be a benefit to doing the conditioning regimen and
    bone marrow transplant separately so that participants would have time to recover
    and heal prior to receiving the kidney transplant.
    9 U.S. National Library of Medicine, Learn About Clinical Studies,
    https://clinicaltrials.gov/ct2/about-studies/learn (last updated Mar. 2019). A Data
    Safety Monitoring Board can recommend to the sponsor that a trial be stopped if it is
    5
    Also, an Institutional Review Board (IRB) reviewed the protocol and consent
    form and monitored the clinical trial.
    When the Shwabs met with Elizabeth Reed to discuss the clinical trial
    initially, Dr. Ravindra was present for part of the discussion. Dr. Ravindra also
    discussed the risks and benefits of the clinical trial. Reed later testified that
    she gave the Shwabs the sixteen-page consent form to take home and read, a
    form which detailed the trial and possible side effects, including cancer,
    infertility and death. She also provided a brochure prepared by Dr. Ildstad
    describing the trial. Mack later claimed that the couple was not given the
    consent form to take with them. At this point the Shwabs expressed interest in
    participating in the trial.
    In their depositions the Shwabs stated that Reed told them that they
    could expect virtually no side effects and that the worst-case scenario was that
    the trial would not work and Brooke would need a traditional kidney
    transplant. Additionally, Brooke testified that no one explained that the
    purpose of the trial was to determine whether the protocol was safe and
    effective. Mack also testified in his deposition that Reed explained that the
    worst that had happened to anyone in the trial was that they had to take more
    anti-rejection medication, but that most people who underwent this process
    ineffective, is harming participants, or is unlikely to serve its scientific purpose. Dr.
    Ildstad testified that the Data Safety Monitoring Board includes highly respected
    experts who are completely independent of the study. The Board routinely meets twice
    a year to review all subject data and study protocols.
    6
    achieved tolerance of the donor kidney. Conversely, Dr. Ravindra testified that
    as of the date of his conversation with the Shwabs, January 24, 2008, no
    participants had achieved tolerance and that he personally gave the Shwabs
    that information.
    Brooke had a follow-up appointment with her nephrologist, Dr. Sanford
    Reikes, who was treating her for end-stage renal disease. They discussed the
    trial and Dr. Reikes described the potential benefits as substantial. He also
    informed Brooke that the risk of recurrence of her particular type of kidney
    disease in the transplanted organ may not be known. The Shwabs had several
    follow-up appointments with Dr. Ravindra in February 2008 primarily focused
    on Mack’s candidacy as a kidney donor. The clinical trial was mentioned at
    these meetings, and Dr. Ravindra encouraged the Shwabs to meet with all of
    the members of the trial before deciding whether to participate.
    On February 26, 2008, the Shwabs met with Dr. Craig Silverman, a
    professor of radiation oncology at the University of Louisville. Dr. Silverman’s
    only involvement in the clinical trial was administering the total body
    irradiation and he did not collaborate with Drs. Ildstad, Ravindra, and Roger
    Herzig in developing the protocol or the sixteen-page informed consent form.
    Dr. Silverman discussed the purpose of the total body irradiation, the
    technique, and the side effects, including potential “second cancers,” such as
    blood cancers, leukemia, lymphomas, and bone cancers. Dr. Silverman had a
    separate consent form, “Explanation of and Consent to Radiation Therapy,” on
    which he handwrote the words “second cancer” during this February 26, 2008
    7
    discussion. Dr. Silverman also provided two pamphlets that detailed radiation
    therapy and total body irradiation, identifying potential side effects, for the
    Shwabs’ review. After this meeting Brooke signed the consent form and agreed
    to participate in the clinical trial.
    The Shwabs also met with Dr. Herzig, a professor of hematology and
    oncology at the University of Louisville and a clinical trial co-investigator, on
    March 10, 2008 for an evaluation and discussion of the trial. Dr. Herzig
    reviewed the trial’s regimen and potential complications with the Shwabs. Dr.
    Herzig indicated that he spent an “extended period of time” with the Shwabs.
    He discussed the clinical trial informed consent form, focusing mostly on the
    portion of the protocol with which he was involved. Following this meeting,
    Brooke signed a revised consent form.10 Excerpts from that consent form
    include:
    The purpose of this study is to determine if this procedure is safe
    . . . . (p. 2)
    This is a Phase I research study. Phase I is research in which the
    safety of the procedure is evaluated. . . . However, the approach in
    this study using X-ray therapy and facilitator cells has not been
    done before. This procedure is investigational, which means it has
    not been approved by the U.S. Food and Drug Administration
    (FDA). (p. 2)
    This combined bone marrow procedure is basically untested in
    humans. . . . The safety and effectiveness of this study procedure
    will be evaluated. . . . (p. 2)
    10 The March 10, 2008 consent form is the most recent version. While Brooke
    originally consented to participate in the trial on February 26, 2008, the consent form
    was amended because the Department of Defense provided funding and free care was
    provided to trial participants at government facilities. The initial consent form
    provided for care at Jewish Hospital. The February 26, 2008 consent form is not in
    the record, but the parties agree the March 10, 2008 consent form is controlling.
    8
    ....
    Presently, drugs are required to prevent rejection of a transplanted
    kidney. The drugs used to treat rejection have many side effects.
    Besides weakening your body’s ability to fight infection, they can
    also cause high blood pressure, kidney damage, and possible
    cancer. (p. 4)
    ....
    Each of the different parts of this study may result in increased
    risks of serious complications, including death. (p. 5)
    ....
    There is also a very low risk of developing cancer related to the
    radiation during the course of your lifetime. (p. 5)
    ....
    It is not possible to be informed of every possible complication or
    risk. (p. 6)
    ....
    Other risks: [associated with the use of Mycophenolate mofetil
    (MMF), an immunosuppressant drug] – lymphoma (cancer of the
    lymph nodes) . . . . (p. 7)
    ....
    There may be unknown risks, which are not known at this time.
    (p. 7)
    ....
    These delayed effects may include certain types of cancer. (p. 8)
    The Shwabs allege that Reed verbally told them they could expect
    virtually no side effects, that the worst-case scenario was that the clinical trial
    would be unsuccessful and that Brooke would have to undergo a traditional
    kidney transplant; that the doctors involved in the trial made similar
    9
    statements or did not discuss the risks at all; and that they were told the
    clinical trial had been successful in five other patients, which was not true.
    Although Mack testified that they were told the trial had achieved success in
    five people,11 Dr. Ildstad testified that at the time Brooke entered the clinical
    trial no participants had achieved the study’s goal of avoiding the need for
    immunosuppressants.
    Brooke began her treatment in the clinical trial in March 2008 and her
    kidney transplant was performed in June 2008. For over a year after the
    transplant, Brooke’s white blood cell count remained low and she continued to
    feel ill. The clinical trial’s medical providers could not determine what was
    wrong, so she travelled to Northwestern University in Chicago to obtain a
    second opinion. There she was diagnosed with MDS. One of the doctors at
    Northwestern University and Dr. Ravindra indicated that the trial could have
    caused the MDS. After seeking treatment for MDS, Brooke learned that her
    body had rejected the kidney transplant she received during the clinical trial.
    On September 2, 2010, the Shwabs filed a complaint against Dr.
    Ravindra, Dr. Silverman, Dr. Herzig, Dr. Ildstad, the University Medical Center
    and the ICT (the medical defendants)12 for negligent failure to adequately
    11  Mack explained that the information about the successes in five people in the
    trial were from various trials. Reed testified that, as a clinical research manager for
    the ICT, she managed four trials—two kidney trials, one heart trial, and a sickle cell
    study at a children’s hospital.
    12 On September 23, 2010, the Shwabs filed a separate action against Jewish
    Hospital claiming negligence, lack of informed consent and loss of spousal consortium.
    On January 10, 2011 that action was consolidated with the Shwabs’ claim against all
    other medical defendants. Jewish Hospital filed a motion for summary judgment on
    October 23, 2014 because none of the individuals involved in the clinical trial were
    10
    inform Brooke of the risks of participating in the clinical trial.13 They claimed
    that had they been properly and adequately informed of the risks, then Brooke
    would not have given consent.
    The Shwabs named two experts in support of their claims. Dr. Lee
    Levitt, a retired board-certified hematologist and oncologist, testified by
    deposition that the informed consent for the trial was deficient. Dr. Levitt
    opined that the Shwabs did not understand the nature of a Phase I clinical trial
    or the potential toxicity of this particular trial. He did not believe that the
    alternatives were highlighted to the extent they should have been. He also
    opined that the informed consent form should have included more specific
    information about the risk of cancer, specifically MDS, and that the informed
    consent process made the risks seem relatively modest. Additionally, Dr. Levitt
    believed that Brooke should have been informed that there were alternatives,
    such as a traditional kidney transplant from her husband in which she had an
    agents or employees of Jewish Hospital. While Jewish Hospital was listed as a site for
    the clinical trial on the informed consent form, the only procedure performed at
    Jewish Hospital was the removal of one of Mack’s kidneys. The Shwabs did not object
    to summary judgment and their claims as to Jewish Hospital were dismissed on
    March 27, 2014.
    13  The Shwabs named the University Medical Center as a defendant in its
    capacity as the James Graham Brown Cancer Center and as the University of
    Louisville Hospital. The ICT filed a motion for summary judgment because it is not a
    separate legal entity. Rather, the ICT is simply a designated institution within the
    University of Louisville itself, approved by the University of Louisville Board of
    Trustees. In short, the ICT is part of the University of Louisville. The Shwabs did not
    oppose the motion. The trial court dismissed the ICT from the action on April 26,
    2012 and Dr. Ildstad, the Director of the ICT, on April 29, 2013. Dr. Ildstad never
    met, treated or had any contact with the Shwabs.
    11
    estimated 85% chance of success, albeit with the necessity of
    immunosuppressant drugs.
    The Shwabs also identified another expert, Dr. Guillermo Garcia-Manero,
    who treated Brooke for MDS at MD Anderson Cancer Center in Houston. His
    testimony focused on the cause of the MDS and he opined that the
    chemotherapy and radiation Brooke underwent in conjunction with the bone
    marrow transplant were most likely the cause. He spoke extensively about the
    difficulty of diagnosing MDS and determining its cause. Dr. Garcia-Manero did
    not testify regarding informed consent.
    On April 21, 2017, the remaining medical defendants collectively filed a
    motion for summary judgment arguing that the Shwabs failed to prove their
    claim of improper informed consent. The defendants asserted that the consent
    form Brooke signed sufficiently informed her of all known or reasonably
    anticipated risks associated with participation in the clinical trial. The Shwabs
    opposed the motion and argued that the adequacy of Brooke’s informed
    consent was a jury question.
    On July 10, 2018, the trial court granted summary judgment in favor of
    the medical defendants. The trial court concluded that the lengthy consent
    form Brooke signed complied with Kentucky statutory authority and federal
    regulations. While the form did not explicitly include MDS as a risk, it stated
    that participation could result in a risk of “various cancers” and listed a
    multitude of risks and side effects. Brooke was given ample opportunity to
    review the form and consult with medical providers prior to giving consent.
    12
    The trial court noted Brooke was the first known individual to have developed
    MDS following participation in the clinical trial or similar study and thus MDS
    was not a reasonably known risk. Because it found no genuine issues of
    material fact regarding her claim that the medical defendants failed to properly
    inform her of the reasonably known risks associated with the clinical trial, the
    trial court granted summary judgment to the defendants.
    The Court of Appeals reversed the trial court’s opinion and order because
    it believed that the Shwabs presented enough evidence to defeat a motion for
    summary judgment. The appellate court focused on the deposition testimony
    of Dr. Levitt, who opined that the medical defendants used a deficient informed
    consent form, a form that should have, but did not, mention certain specific
    risks, such as stem cell damage, leukemia and MDS. He also claimed that
    MDS is a known side effect when total body irradiation and chemotherapy are
    used in conjunction. While the medical defendants presented evidence to the
    contrary, the Court of Appeals concluded that conflicting evidence made the
    adequacy of the informed consent an issue for the jury. Additionally, that
    court noted that the Shwabs testified that no one explained the possibility that
    there could be extreme risks associated with the trial and that they were only
    told that, at worst, the trial would not work. Ultimately the Court of Appeals
    concluded that the Shwabs presented enough evidence to potentially convince
    a jury that the medical defendants did not give them enough information to
    reasonably understand the trial or the potential risks.
    13
    Having granted discretionary review, heard oral arguments and carefully
    considered the record, we reverse the Court of Appeals.14 Given the
    undisputed facts and applicable law, the trial court properly granted summary
    judgment.
    ANALYSIS
    On appeal, we review a summary judgment de novo. Shelton v. Ky.
    Easter Seals Soc’y, Inc., 
    413 S.W.3d 901
    , 905 (Ky. 2013). We must consider
    whether the trial court “correctly determined that there were no genuine issues
    of material fact and that the moving party was entitled to judgment as a matter
    of law.” Fluke Corp. v. LeMaster, 
    306 S.W.3d 55
    , 59 (Ky. 2010). To defeat
    summary judgment, the Shwabs must have presented affirmative evidence that
    a genuine issue of material fact exists. Steelvest, Inc. v. Scansteel Serv. Ctr.,
    Inc., 
    807 S.W.2d 476
    , 480 (Ky. 1991).
    Turning to the substantive law of informed consent, “it is a well-
    established principle of law that, as an aspect of proper medical practice,
    physicians have a general duty to disclose to their patients in accordance with
    accepted medical standards the risks and benefits of the treatment to be
    performed.” Sargent v. Shaffer, 
    467 S.W.3d 198
    , 206 (Ky. 2015). KRS 304.40-
    320 provides the informed consent standard:
    In any action brought for treating, examining, or operating on a
    claimant wherein the claimant’s informed consent is an element,
    the claimant’s informed consent shall be deemed to have been
    given where:
    14 Dr. Ravindra did not move this Court for discretionary review and is not a
    party in this appeal.
    14
    (1) The action of the health care provider in obtaining the consent
    of the patient or another person authorized to give consent for the
    patient was in accordance with the accepted standard of medical
    or dental practice among members of the profession with similar
    training and experience; and
    (2) A reasonable individual, from the information provided by the
    health care provider under the circumstances, would have a
    general understanding of the procedure and medically or dentally
    acceptable alternative procedures or treatments and substantial
    risks and hazards inherent in the proposed treatment or
    procedures which are recognized among other health care
    providers who perform similar treatments or procedures . . . .15
    (Emphasis added.) Examining the contours of informed consent, this Court
    has noted that “[t]he two subsections perform very different functions and
    address two different aspects of ‘informed consent.’” Sargent, 467 S.W.3d at
    209. A physician must comply with both subsections in order to satisfy the
    statutory standard for obtaining informed consent. Id. at 207. Therefore, a
    breach of the statutory standard for informed consent can be established by
    proving that a medical care provider failed to meet either subsection of KRS
    304.40-320. Argotte v. Harrington, 
    521 S.W.3d 550
    , 556 (Ky. 2017).
    I. The Actions of the Medical Care Providers Satisfied Subsection
    One of the Informed Consent Statute.
    The requirements of each subsection of KRS 304.40-320 were explained
    in Sargent, 467 S.W.3d at 209 (quoting KRS 304.40-320(1)):
    Subsection (1) covers the means employed by the health care
    provider to obtain the patient’s consent. The “action of the health
    care provider” in obtaining consent must be “in accordance with
    15 KRS 304.40-320(3) provides requirements for obtaining informed consent in
    emergency situations; that subsection is inapplicable in this case.
    15
    the accepted standards of [the relevant] medical or dental
    practice[.]”
    Thus, to meet the requirements of the first subsection the Shwabs must show
    that the process by which the medical defendants obtained her consent did not
    comply with “accepted standards” within the medical profession.
    As this Court has expressly recognized, informed consent “is a process,
    not a document.” Kovacs v. Freeman, 
    957 S.W.2d 251
    , 254 (Ky. 1997). Over
    the course of several weeks in early 2008 Brooke met with five medical care
    providers, four providers associated with the clinical study plus her own
    nephrologist, for what the medical defendants estimate was a total of 120
    minutes. During these meetings Brooke was informed of the trial’s lack of
    success, substantial risks, and potential complications. The Shwabs also had
    the opportunity to ask questions and receive answers from the medical
    specialists. In addition, during their initial discussions about the clinical trial,
    they were given the detailed informed consent form to take home and review.16
    Although informed consent is a process, the detailed informed consent
    document Brooke signed is highly relevant in our analysis.
    The existence of a signed consent form gives rise to a
    presumption that patients ordinarily read and take whatever
    other measures are necessary to understand the nature,
    terms and general meaning of consent. To hold otherwise
    would negate the legal significance to written consent forms
    16  As noted, Mack disputes that they were allowed to take the consent form
    home. Reed testified that she gave it to them because it was required by the protocol
    for the clinical trial. Dr. Ravindra also testified that providing a copy of the consent
    form was part of Reed’s typical routine when explaining the clinical trial to a
    candidate.
    16
    signed by the patient and render the consent form
    completely unreliable.
    Hoofnel v. Segal, 
    199 S.W.3d 147
    , 151 (Ky. 2006).17 Our review of the record
    reflects that Brooke had ample opportunity to review the consent form and
    ensure that she understood its contents.
    Dr. Ravindra met with the Shwabs on January 24, 2008 to
    discuss Brooke’s candidacy for a kidney transplant. Dr. Ravindra
    described the Shwabs as “very intelligent, very sharp” people. As noted,
    Mack’s mother first brought up the trial, stating that she heard about it
    on the radio. Dr. Ravindra later testified that he explained chimerism,18
    avoiding immunosuppression and that chimerism was not achieved in
    the nine participants who had taken part in the clinical trial. He recalled
    that the Shwabs had concerns about graft versus host disease and he
    explained that it was a serious complication and that their fears were
    genuine. Dr. Ravindra also encouraged the Shwabs to meet with Dr.
    Herzig and Dr. Silverman to help ensure they understood the clinical
    trial prior to deciding on whether to participate. In his second meeting
    with the Shwabs, the Shwabs asked a number of questions about what
    Mack would have to do for the trial. Dr. Ravindra testified that at the
    time he ceased his involvement in the clinical trial when he left for a
    position at Duke University it was unclear whether MDS was related to
    the trial.
    Elizabeth Reed met with the Shwabs to discuss the clinical trial
    on January 24, 2008, with Dr. Ravindra present for part of that initial
    meeting. Reed was the trial’s clinical research manager, having been in
    that role for a few months following prior experience at Jewish Hospital
    and eighteen years at the Kentucky Organ Donor Affiliates. She recalled
    17 While Hoofnel involved a claim of medical battery arising from surgery for
    removal of a colon tumor wherein the patient disputed also giving consent for removal
    of her ovaries and uterus if necessary, this recognition of the importance of an
    informed consent document applies equally in a medical negligence/informed consent
    case. The consent form signed by Brooke is crucial to the analysis of the informed
    consent process.
    18 Chimerism means that the transplant recipient has a mixture of the donor
    and recipient’s immune systems. The informed consent form explains that Brooke
    would receive a stem cell transplant from her kidney donor, Mack. Therefore, Brooke
    would have two types of bone marrow, hers and Mack’s, called “mixed chimerism.”
    See also Stedmans Medical Dictionary (2014) (“Chimerism” is defined as “the state of
    being chimera” and “chimera” is defined as “[a]n organism that has received a
    transplant of genetically and immunologically different tissue, such as bone marrow.).
    17
    this first meeting and stated that she had the informed consent form
    with her because she used it as an educational tool to describe the trial.
    The Shwabs asked Reed questions and she estimated that she spent
    fifteen to twenty minutes with them this first time. Reed testified that
    she discussed the risks listed in the informed consent form in great
    detail and emphasized to the Shwabs that in a Phase I trial the
    researchers do not know what may happen. Importantly, she testified
    that she gave the Shwabs the informed consent form to take home and
    read because their protocol required her to do so. She explained that,
    because it was a Phase I clinical trial with unknown risks, it was
    important that patients fully understand the informed consent. She also
    gave them the brochure created by Dr. Ildstad that described the clinical
    trial.
    Reed denies that she ever told the Shwabs that the worst thing
    that could happen is that the protocol would not work, and that Brooke
    would have to take anti-rejection medication. She estimated that on
    March 10, 2008 when she met with Brooke to sign the consent form that
    the process took approximately one hour. When questioned about her
    knowledge regarding obtaining informed consent, Reed also explained
    that before she began managing the study she was given the trial
    protocol and informed consent form, reviewed it, and was able to ask her
    predecessor questions about it. Reed also shadowed her predecessor
    while she obtained informed consent for the various clinical trials
    sponsored by the ICT. She had received additional training on how to
    obtain informed consent from Jewish Hospital and her former employer,
    Kentucky Organ Donor Affiliates. She also had discussed the clinical
    trial protocol and informed consent process during meetings with Drs.
    Ildstad, Ravindra and Herzig.
    Dr. Herzig testified that when he met with Brooke he reviewed
    issues with her that were included in the informed consent. On the day
    Brooke signed the consent form Dr. Herzig meet with her for an
    “extended period of time.” He described the process and explained that
    when he met with the Shwabs on March 10, 2008 they had already met
    with Dr. Ravindra and discussed the protocol. He explained the trial’s
    regimen to the Shwabs and discussed the potential complications
    involved. He also explained that the protocol had not yet been
    successful. As for his training in the informed consent process generally,
    he also testified that he had discussions with Dr. Ildstad, Dr. Ravindra
    and Reed about how to obtain informed consent for the trial.
    Dr. Silverman testified that he had a lengthy discussion with
    Brooke about the purpose, technique and side effects of radiation. Dr.
    Silverman testified that it was routine procedure to give patients two
    pamphlets, one that detailed the radiation procedure and another
    pamphlet that discussed total body irradiation (TBI). The TBI pamphlet
    listed “second cancer” as a possible side effect. The purpose of providing
    the pamphlets was to allow patients to take the materials home to review
    18
    and ask questions prior to the procedure. Dr. Silverman specifically
    wrote “second cancer” on the list of possible side effects in the TBI
    consent form and stated that the risk of a second cancer was one of the
    many things he explained to Brooke.19
    Dr. Levitt, the only expert witness the Shwabs disclosed relating to the
    consent process, provided his opinions about the informed consent form and
    process. He stated that written consent is required but that there should also
    be a detailed oral conversation with the patient that describes the risks and
    benefits of a procedure, as well as available alternatives. Dr. Levitt testified
    that these components of obtaining informed consent are even more important
    in the context of a Phase I clinical trial. He testified that he believed the
    medical defendants in this case used a flawed written consent form because it
    was too lengthy and difficult to follow. Conversely, Dr. Levitt further opined
    that the form was not detailed enough because it should have mentioned
    specific risks regarding bone marrow, including stem cell damage, leukemia
    and MDS. He claimed that MDS is a known side effect when total body
    irradiation and chemotherapy are used in conjunction and therefore the risk
    should have been included in the consent form.
    Most of Dr. Levitt’s criticism of Brooke’s consent to participate in the trial
    stems from the Shwabs’ testimony that they were not given all the necessary
    information and simply did not understand the extent of the risks. Notably,
    19 “Second cancer” was referenced because Dr. Silverman primarily used total
    body irradiation for patients with either advanced lymphoma or leukemia. Brooke was
    one of only three non-cancer patients he had ever treated with TBI. In twenty-two
    years of administering TBI he had never seen a patient develop a second cancer.
    19
    Dr. Levitt did not criticize how the medical defendants conducted the consent
    process but instead focused his deposition testimony on the content of the
    information as described by the Shwabs in their respective depositions.
    In essence, Dr. Levitt believed the Shwabs came away with the idea that
    there was not much bad that could happen from the trial. However, they
    received, reviewed and signed the consent form that listed numerous potential
    risks and side effects, making it difficult to conceive how the Shwabs (or
    anyone for that matter) could believe nothing bad could happen. The
    numerous listed risks and side effects also make it difficult to conceive that any
    of the medical care providers they met with would have told them nothing bad
    would happen, especially given the definition and very nature of a Phase I
    clinical trial. As the first page of text in the consent form relates, the trial was
    to evaluate “the safety of the procedure”; “the approach . . . has not been done
    before”; the “procedure is investigational” and therefore not approved by the
    FDA; and the “combined bone marrow procedure is basically untested in
    humans.”
    Leaving aside Dr. Levitt’s primary reliance on the Shwabs’ deposition
    testimony, his review of the informed consent process was largely incomplete.
    While Dr. Levitt reviewed the Shwabs’, Dr. Garcia-Manero’s and Elizabeth
    Reed’s depositions, he acknowledged that he did not read Drs. Ravindra’s,
    Herzig’s, Silverman’s and Ildstad’s depositions. As noted supra, the Shwabs
    also met with Dr. Silverman, Dr. Herzig and Dr. Ravindra to discuss the trial
    before Brooke consented to participate and all of these individual defendants
    20
    were deposed. Dr. Ildstad, the trial’s sponsor involved with drafting the
    consent form and materials about the clinical trial, was also deposed. Dr.
    Levitt did not consider any of these fact witnesses’ depositions and thus was
    unaware of Drs. Ravindra’s, Herzig’s and Silverman’s sworn testimony
    regarding their conversations with the Shwabs. When questioned, he admitted
    that review of those depositions “could be” pertinent to his opinion regarding
    the discussions they had with the Shwabs about the clinical trial and risks. He
    even agreed that it would be important to know what everyone says about the
    consent process, not just the Shwabs. Although Reed engaged in discussions
    with the Shwabs about the clinical trial and was important to the informed
    consent process, she did not operate solo. Significantly, Dr. Levitt failed to
    review the depositions of the three medical care providers who discussed the
    clinical trial with the Shwabs, all of whom were deposed at least three years
    prior to Dr. Levitt.
    Returning to the law of informed consent, the crucial component of a
    claim under KRS 304.40-320(1) is evidence that a medical care provider’s
    actions did not comply “with the accepted standard of medical or dental
    practice among members of the profession with similar training and
    experience.” “Ordinarily, the failure to comply with a medical profession
    standard can only be proven by expert testimony.” Argotte, 521 S.W.3d at 556.
    While Dr. Levitt expressed his own personal criticism of the informed consent
    form and process, i.e., the informed consent form does not give a patient a
    sense of the degree of risk involved and MDS specifically should have been
    21
    included as a risk and discussed with the Shwabs, he did not testify to an
    accepted standard of medical practice and thus did not testify as to a breach of
    that standard. It was incumbent upon the Shwabs to “show the physician’s
    actions for obtaining consent fell outside ‘the accepted standard of medical . . .
    practice.’” Argotte, 521 S.W.3d at 556 (quoting KRS 304.40-320(1)). In
    addition to not testifying that the medical defendants deviated from an
    accepted standard of care, Dr. Levitt lacked a proper basis for such testimony
    given that he did not review depositions of three medical defendants (in fact the
    three physicians involved) who discussed the clinical trial with Brooke and
    actually provided medical treatment pursuant to the clinical trial protocol.
    While Dr. Levitt noted his substantial clinical trial experience, including
    his participation in trials that studied leukemia and MDS, he was unable to
    specifically cite any medical literature to support his assertions that the
    informed consent process was deficient. The medical defendants’ counsel
    specifically asked Dr. Levitt for citations to medical literature that more
    accurately reflected the risk of MDS or leukemia. Dr. Levitt stated that he had
    not “specifically reviewed the medical literature with regard to this” but that
    textbooks on radiation medicine reviewed data on total body irradiation, MDS
    and leukemia. He generally referenced studies that reviewed the incidence of
    MDS and the increase in incidence when chemotherapy is added. He also
    suggested that “most of the literature” indicates that the combination of total
    body irradiation and chemotherapy causes an increased risk of leukemia and
    MDS but did not cite any particular medical treatise or publication.
    22
    Stated simply, Dr. Levitt’s testimony failed to qualify as expert testimony
    necessary to satisfy KRS 304.40-320(1). He did not possess all the relevant
    information regarding the various discussions with medical care providers and
    instead resorted almost entirely to the Shwabs’ testimony regarding the
    informed consent process. KRS 304.40-320(1) requires more than one
    physician’s personal opinion regarding how he believes informed consent
    should work. Dr. Levitt’s testimony simply does not constitute evidence that
    “the [medical defendants’] actions for obtaining consent fell outside ‘the
    accepted standard of medical . . . practice.’” Argotte, 521 S.W.3d at 556
    (quoting KRS 304.40-320(1)).
    While the Shwabs did not meet their burden under KRS 304.40-320(1),
    we note that it would be a difficult task for any plaintiff given the extra vetting
    that occurs where informed consent is sought in the context of a clinical trial
    subject to federal regulation. Title 21 C.F.R. § 50.25 outlines the information
    that must be contained within a valid informed consent form:
    (a) Basic elements of informed consent. In seeking informed
    consent, the following information shall be provided to each
    subject:
    (1) A statement that the trial involves research, an
    explanation of the purposes of the research and the expected
    duration of the subject’s participation, a description of the
    procedures to be followed, and identification of any
    procedures which are experimental.
    (2) A description of any reasonably foreseeable risks or
    discomforts to the subject.
    (3) A description of any benefits to the subject or to others
    which may reasonably be expected from the research.
    23
    (4) A disclosure of appropriate alternative procedures or
    courses of treatment, if any, that might be advantageous to
    the subject.
    (5) A statement describing the extent, if any, to which
    confidentiality of records identifying the subject will be
    maintained and that notes the possibility that the Food and
    Drug Administration may inspect the records.
    (6) For research involving more than minimal risk, an
    explanation as to whether any compensation and an
    explanation as to whether any medical treatments are
    available if injury occurs and, if so, what they consist of, or
    where further information may be obtained.
    (7) An explanation of whom to contact for answers to
    pertinent questions about the research and research
    subjects’ rights, and whom to contact in the event of a
    research-related injury to the subject.
    (8) A statement that participation is voluntary, that refusal to
    participate will involve no penalty or loss of benefits to which
    the subject is otherwise entitled, and that the subject may
    discontinue participation at any time without penalty or loss
    of benefits to which the subject is otherwise entitled.
    (Emphasis added.) The clinical trial Brooke participated in would not have
    been allowed to proceed absent compliance with this regulation. Particularly of
    note in the context of this litigation is subsection (2) requiring disclosure of all
    “reasonably foreseeable risks.”
    As for the particular informed consent form Brooke signed, the record
    reflects that Dr. Ildstad, Dr. Ravindra and Dr. Herzig collaborated to draft the
    consent form at an eighth-grade reading level to make it easy to understand.
    The initial draft of the consent form was then provided to the FDA for review.
    The form was next sent to a local IRB, which is a group formally designated to
    24
    review and monitor biomedical research involving human subjects.20 An IRB
    has the authority to approve, require modifications, or disapprove research.
    The U.S. Department of Defense’s own IRB also reviewed the informed consent
    form because the Department of Defense provided funding for the clinical trial.
    The Department of Defense reviewed the consent form and trial protocol to
    ensure both were in accordance with federal regulations.
    Dr. Ildstad’s testimony that the informed consent form was “very
    thoroughly reviewed” through a “very tedious process” is not surprising given
    the various layers of oversight in a clinical trial. In sum, Brooke signed a
    consent form that was drafted and reviewed not only by three medical care
    providers in Kentucky but also reviewed and approved by the FDA, two IRBs
    and the U.S. Department of Defense. Given these circumstances, the prospect
    of a deficient informed consent form that did not conform with the “accepted
    standard of medical . . . practice,” KRS 304.40-320(1), is miniscule, at best. In
    any event, the record reflects no expert testimony regarding the accepted
    standard of medical practice and a breach of that standard and, as a result,
    the trial court properly granted summary judgment as to the medical
    defendants’ compliance with KRS 304.40-320(1).
    20  Institutional Review Boards Frequently Asked Questions, FDA (January 1998),
    https://www.fda.gov/regulatory-information/search-fda-guidance-
    documents/institutional-review-boards-frequently-asked-questions. The local IRB
    that reviewed the informed consent is based in Olympia, Washington and serves as the
    IRB for the University of Louisville.
    25
    II. The Information Conveyed by the Medical Defendants
    Satisfied Subsection Two of the Informed Consent Statute.
    KRS 304.40-320(2) requires that the medical defendants provide
    information that would give “a reasonable individual . . . a general
    understanding of the procedure” and also “medically . . . acceptable alternative
    procedures or treatments and substantial risks and hazards inherent in the
    proposed treatment” as “recognized among other health care providers who
    perform similar treatments or procedures.” The Sargent Court explained that
    [s]ubsection (2) covers the content of “the information
    provided,” and it sets forth the objective standard that “a
    reasonable individual” must have from that information a
    “general understanding” of the risks “recognized among
    health care providers who perform similar
    treatments[.]” KRS 304.40-320(2).
    467 S.W.3d at 209 (emphasis added). Pursuant to the statute the medical
    defendants were required to inform Brooke of the substantial risks inherent in
    the clinical trial treatment and the information provided must be evaluated
    from the standpoint of “a reasonable individual,” not Brooke’s subjective
    understanding or memory.
    The consent form warned that “[t]here may be unknown risks, which are
    not known at this time”; “[i]t is not possible to be informed of every possible
    complication or risk”; that the procedure was “basically untested in humans”;
    that she would “be one of the first groups to be treated”; and that “the
    approach in this trial using X-ray therapy and facilitator cells has not been
    done before.” (pp. 2, 6 and 7.) The consent form further plainly identified
    cancer as a potential risk of the trial, including listing cancer as a risk under
    26
    the total body irradiation section as well as the stem cell transplantation
    section of the consent form. The form also included the following statements:
    [b]esides weakening your body’s ability to fight infection, they can
    also cause high blood pressure, kidney damage, and possibly
    cancer. (p. 4)
    ....
    There is also a very low risk of developing a cancer related to the
    radiation during the course of your lifetime. This risk is estimated
    based on studies of one time exposure to low levels of radiation to
    be less than or equal to 2%. (p. 5)
    ....
    These delayed effects may include certain types of cancer. (p. 8)
    (emphasis added). The form specifically informed the Shwabs that
    participation in the trial was voluntary and that they could “choose not to enter
    the trial and instead receive standard therapy” for Brooke’s condition. In the
    separate consent form for the radiation therapy Brooke acknowledged that
    “second cancer” was a potential risk of the treatment. From an objective
    viewpoint, the multiple references during the consent process through the
    written form and discussions adequately conveyed that cancer was a risk of the
    treatment protocol.
    The fact that MDS was not specifically listed in the consent form, despite
    Dr. Levitt’s testimony that it should have been included as a risk, does not
    render the informed consent invalid. No other patient who participated in the
    trial had developed MDS.21 Additionally, expert testimony established that
    21 The Shwabs assert that Brooke was the very first research subject in this
    Phase I clinical trial. At the time Brooke participated in the trial it had been ongoing
    since 2003 and had ten to twelve participants prior to Brooke. When Brooke
    27
    MDS is typically developed by older males, not young females like Brooke. The
    Shwabs’ own expert witness, Dr. Garcia-Manero, testified that “not everyone
    that is exposed to these chemoradiation therapies will get this disorder. . . . It’s
    actually a minority” of “less than five percent of patients.” The Leukemia and
    Lymphoma Society states that, “[a] small number of patients who have received
    chemotherapy and/or radiation therapy in the past for another cancer have a
    small risk of developing treatment-related MDS. Generally, the chance of
    developing a myelodysplastic syndrome as a result of treatment for another
    cancer is very low.”22 Given the low prevalence of MDS and the fact that no
    other patient in the trial or similar studies had developed MDS, this specific
    cancer could not constitute a substantial risk under Kentucky informed
    consent law and, in fact, no expert testified as such.23
    The Shwabs insist that the issue of “substantial risk” is for the jury and
    does not require expert testimony. We briefly review the two cases relied on to
    clarify the law. In Sargent, the trial court erroneously instructed the jury by
    failing to incorporate the requirements of KRS 304.40-320 applicable to a
    medical provider’s duty to obtain informed consent. 467 S.W.3d at 212. The
    participated in the trial in 2008 she was the first subject under the particular protocol
    which used the sequential method of total body irradiation and fludarabine.
    22Myelodysplastic Syndromes, LEUKEMIA AND LYMPHOMA SOCIETY,
    https://www.lls.org/booklet/myelodysplastic-syndromes (last updated 2019).
    23 See Goodman v. U.S., 
    298 F.3d 1048
    , 1058 (9th Cir. 2002), where a clinical
    research study participant was not informed of the complication from which she
    ultimately died. The federal appellate court held that the physicians had no reason to
    know there was a risk of that complication as no study participants had previously
    suffered that complication. The record supported “the conclusion that the NIH doctors
    were not, and could not reasonably have been, aware . . .” of the unperceived risk. 
    Id. 28
    Court explained that jurors can apply the “reasonable individual” and “general
    understanding” standards provided in subsection (2) of KRS 304.40-320, but
    that “evidence on whether the ‘risks and hazards’ involved are among those
    ‘recognized among other health care providers who perform similar treatments
    or procedures’” is required. 
    Id. at 209
    . Notably, the majority in Sargent failed
    to state “substantial risks and hazards,” the language of the statute, in
    explaining what is required in the medical evidence. This Court’s reference to
    the ability of the jurors to apply the law, moreover, was focused on determining
    if a reasonable individual would have a general understanding of the
    information provided not on their ability to know whether a particular risk was
    substantial or not. In Argotte, a 4-3 decision, the majority stated that proving
    a failure to comply with KRS 304.40-320 “requires an expert opinion only as
    needed to establish “whether the ‘risks and hazards’ involved [in the plaintiff’s
    claim] are among those ‘recognized among other health care providers who
    perform similar treatments or procedures.’” 521 S.W.3d at 556 (quoting KRS
    304.40-320(2)). Once again the majority omitted “substantial,” which is crucial
    to correct application of the statute.
    As Justice Keller explained in a separate opinion (joined by two other
    Justices) in Argotte, KRS 304.40-320(2) expressly states that the risks to be
    disclosed must have been “substantial risks.” 521 S.W.3d at 562 (Keller, J.,
    concurring in part and dissenting in part). The dissenters did not believe “a
    jury of laypersons, without guidance from providers who perform similar
    treatments or procedures, i.e., expert witnesses, can independently determine
    29
    whether a risk is substantial.” Id. Indeed, determining whether a particular
    risk is substantial is not only a matter best addressed by the medical
    community and therefore an element requiring expert testimony, but that is
    what a plain reading of KRS 304.40-320(2) requires, i.e., “substantial risks and
    hazards inherent in the proposed treatment or procedures which are
    recognized among other health care providers who perform similar treatments
    or procedures.” To the extent that Sargent and Argotte suggest that the
    substantiality of a risk is a jury question that does not depend on medical
    evidence those holdings are overruled. Under the informed consent statute,
    the Shwabs’ claim, premised on a failure to disclose the risk of MDS, required
    expert testimony establishing that MDS was a recognized substantial risk and
    they had no such testimony. In any event, to the extent that cancer generally
    was a substantial risk associated with the treatment in the clinical trial, that
    risk was appropriately disclosed numerous times.
    Dr. Levitt testified that the Shwabs did not understand the risks involved
    in the clinical trial, relying on the Shwabs’ subjective testimony. In Sargent,
    however, this Court emphasized that subsection (2) of KRS 304.40-320 creates
    an objective standard: “Meeting the standard does not require that
    patient’s actual understanding of the risks; it only requires that the risks be
    explained so that ‘a reasonable individual’ would gain a general understanding
    of the risks.” 467 S.W.3d at 208 n.10. Thus our informed consent law does
    not require a determination of how the plaintiff-patient claims to have
    understood the consent form, procedure and risks but rather how a reasonable
    30
    person would have understood the information.24 Consequently, the standard
    in subsection (2) is not met by a plaintiff-patient, after the fact, simply claiming
    they were not properly informed or that, had they known of the specific risk
    that resulted in actual harm, they would not have consented to the treatment
    or procedure.25
    As noted in the concurring in result only opinion in Sargent, 467 S.W.3d
    at 218, KRS 304.40–320 was enacted as part of a tort-reform effort and was
    produced by the Governor’s Hospitals and Physicians Professional Liability
    Insurance Advisory Committee in 1975. In the Committee’s Majority Report,
    they describe the statute (Section 13 of their proposal and eventually Section 4
    of Senate Bill 248 in the 1976 Session of the General Assembly) as follows:
    This section will legislatively require that “informed consent” cases
    be proven by expert testimony relating to accepted standards of
    practice of the profession in providing information, and further
    require that an objective standard be applied in determining
    whether that information would likely have resulted in any
    different decision by the plaintiff. The purpose of this section is to
    eliminate the possibility of (1) a jury’s speculating after the fact
    that the health care provider should have told the plaintiff of a
    given risk even though accepted professional standards would not
    require such advance information, and (2) a plaintiff's testifying
    24Some jurisdictions have held that under an objective approach, a patient’s
    hindsight testimony is relevant, but not controlling. See Goldberg v. Boone, 
    912 A.2d 698
    , 702 (Md. 2006); Roybal v. Bell, 
    778 P.2d 108
    , 112 (Wyo. 1989).
    25  If the informed consent standard were subjective then a plaintiff-patient’s
    testimony would control. Proof of causation, i.e., that adequate disclosure would have
    caused the patient to decline treatment because of the risk that resulted in actual
    harm, viewed under a subjective standard “would ultimately turn on the credibility of
    the hindsight of a person seeking recovery after he had experienced a most
    undesirable result. Such a test puts the physician in ‘jeopardy of the patient’s
    hindsight and bitterness.’” Sard v. Hardy, 
    379 A.2d 1014
    , 1025 (Md. App. 1977)
    (quoting Canterbury v. Spence, 
    464 F.2d 772
    , 790-91 (D.C. Cir. 1972)) (internal
    citation omitted).
    31
    that had he known of an unforeseeable or unlikely injury he would
    not have consented to the recommended health care.
    As this passage reflects, the informed consent statute was enacted, at least in
    part, to prevent the type of hindsight scenario present in this case.
    The Shwabs did not present evidence that the information given to
    Brooke failed to provide a reasonable person a “general understanding” of any
    “substantial risks” that were “recognized among other health care providers”
    performing similar research and treatment. Moreover, our own review, like the
    trial court’s, satisfies us that no issue of material fact exists as to the
    applicability of subsection (2) of KRS 304.40-320 to this case. MDS was not a
    “substantial risk” at the time Brooke entered the trial given its low prevalence
    generally in young females, and the fact that no other patient in the clinical
    trial or similar study had developed MDS. In any event, a reasonable person
    would certainly understand from even a casual reading of the informed consent
    form that developing cancer (of which MDS is one type) was a risk of the
    clinical trial procedure and treatment.
    III. KRS 304.40-320 Is Clear in Its Application to Any Action
    Wherein Informed Consent Is an Element and Thus Applies Even if
    Medical Treatment Occurs in a Clinical Trial.
    The medical defendants and amici curiae American Medical Association
    and Kentucky Medical Association emphasize the importance of clinical trials
    for the advancement of medicine and the chilling effect that a subjective
    approach to liability, as reflected in the Court of Appeals’ opinion in this case,
    would have on medical professionals’ participation in studies essential for
    improving medical care. In recognition of the unique nature of clinical trials,
    32
    the medical defendants encourage this Court to conclude that Kentucky’s
    informed consent law does not apply to clinical trials because no physician-
    patient relationship exists. We decline because we conclude that a physician-
    patient relationship clearly does exist, at least in the circumstances presented
    here, and our Kentucky informed consent law, tied to standards of accepted
    medical practice and an objective assessment of the information provided to
    the patient, adequately protects the interests of both patients and medical care
    professionals participating in a clinical trial.
    In Greenberg v. Miami Children’s Hospital Research Institute, Inc., the
    case relied on by the medical defendants, the federal court observed that
    “[m]edical consent law does not apply to medical researchers.” 
    264 F. Supp. 2d 1064
    , 1069 (S.D. Fla. 2003). However, the facts of that case are significantly
    different from cases such as this one which entail receiving medical treatment
    in the context of a clinical trial. Greenberg involved the families of children
    with a rare genetic condition who donated tissue samples to a medical
    researcher in hopes of identifying the gene responsible for their disorder. 
    Id. at 1066
    . Once the researcher identified the genes, he applied for a patent and
    began restricting any activity related to the disorder, including testing,
    treatments and research. 
    Id. at 1067
    . The Greenberg plaintiffs filed suit
    alleging they were never informed that the medical researcher intended to seek
    a patent on the research or of his intentions to commercialize the research. 
    Id. at 1068
    . The suit included a claim of lack of informed consent, among other
    claims. 
    Id.
     The court acknowledged that the question of informed consent in
    33
    the context of medical research was relatively novel in Florida but concluded
    that while “in certain circumstances a medical researcher does have a duty of
    informed consent” no such duty existed there. 
    Id. at 1070
    . The Shwabs assert
    that Greenberg is inapplicable because it involved a dispute over financial
    proceeds of non-therapeutic testing. 
    Id. at 1068-69
    . We agree Greenberg is
    distinguishable and find the Kentucky informed consent statute on its face
    applies to a clinical trial involving medical treatment.26
    The informed consent statute plainly applies to “any action brought for
    treating, examining, or operating on a claimant wherein the claimant’s
    informed consent is an element.” KRS 304.40-320 (emphasis added). KRS
    304.40-260(4) includes “patient” in its definition of “claimant” and “patient” is
    defined as “a natural person who receives health care from a licensed health
    care provider under a contract, express or implied.” KRS 304.40-260(3).
    Health care is defined as “any act, or treatment performed or furnished, or
    which should have been performed or furnished, by any health care provider to
    a patient during that patient’s care, treatment, or confinement for a physical or
    mental condition. . . .” KRS 304.40-260(7).
    Brooke qualifies as a claimant and the treatment she received during the
    clinical trial undeniably constitutes health care. The language in KRS 304.40-
    26The Court of Appeals declined to review this issue, stating that it was not
    decided upon by the trial court and citing Fischer v. Fischer, 
    197 S.W.3d 98
    , 102 (Ky.
    2006). While the trial court did not discuss this issue in its order granting summary
    judgment, the medical defendants presented the argument in their motion for
    summary judgment and the issue has been briefed to this Court.
    34
    320 and 304.40-260 is clear and unequivocal. Where a statute is clear and
    unambiguous, “we are not free to construe it otherwise . . . .” MPM Fin. Grp.,
    Inc. v. Morton, 
    289 S.W.3d 193
    , 197 (Ky. 2009). While the Kentucky General
    Assembly could have deferred to federal authorities such as the FDA in
    defining the informed consent duty in a clinical trial or articulated a different
    standard for informed consent in clinical trials, it did not. Because the
    judiciary’s role in statutory construction cases is to see that “the will of the
    legislature” is applied, Allstate Ins. Co. v. Smith, 
    487 S.W.3d 857
    , 861 (Ky.
    2016), we decline to impose a different standard of informed consent for clinical
    trials.
    CONCLUSION
    As the trial court stated in its order granting summary judgment, this is
    “an unquestionably tragic situation for Ms. Shwab and her family,” but for the
    reasons we have discussed the Shwabs do not have a viable informed consent
    claim under Kentucky law. Thus, we reverse the Court of Appeals and remand
    to the trial court for reinstatement of the summary judgment in favor of the
    Appellants.
    All sitting. All concur.
    35
    COUNSEL FOR APPELLANTS:
    Allison Olczak Wildman
    Joseph Andrew Wright
    Thompson Miller & Simpson PLC
    COUNSEL FOR APPELLEES:
    David Brooks Gray
    Gray Law, PLLC
    COUNSEL FOR AMICUS CURIAE,
    KENTUCKY DEFENSE COUNSEL
    INC.:
    Patricia Colleen LeMeur
    Phillips Parker Orberson Arnett, PLC
    COUNSEL FOR AMICI CURIAE,
    THE AMERICAN MEDICAL
    ASSOCIATION AND THE
    KENTUCKY MEDICAL
    ASSOCIATION:
    Bethany A. Breetz
    Sarah Cronan Spurlock
    Stites & Harbison, PLLC
    Philip S. Goldberg
    Shook, Hardy & Bacon LLP
    36