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Addressing ethical and laboratory challenges for initiation of a rapid whole genome sequencing program

Published online by Cambridge University Press:  09 August 2021

Sabrina Malone Jenkins ,
Rachel Palmquist ,
Ashley L. Kapron ,
Carrie Torr ,
D. Hunter Best ,
Mary Anne Karren ,
Luca Brunelli ,
Mark Yandell ,
Martin Tristani-Firouzi  and
David Dimmock
...Show all authors
Sabrina Malone Jenkins*
Affiliation:
Division of Neonatology, Department of Pediatrics, University of Utah School of Medicine, Salt Lake City, UT, USA
Rachel Palmquist
Affiliation:
Division of Pediatric Neurology, Department of Pediatrics, University of Utah School of Medicine, Salt Lake City, UT, USA Primary Children’s Center for Personalized Medicine, Salt Lake City, UT, USA
Ashley L. Kapron
Affiliation:
Center for Genomic Medicine, University of Utah Health, Salt Lake City, UT, USA
Carrie Torr
Affiliation:
Division of Neonatology, Department of Pediatrics, University of Utah School of Medicine, Salt Lake City, UT, USA
D. Hunter Best
Affiliation:
ARUP Institute for Clinical and Experimental Pathology, ARUP Laboratories, Salt Lake City, UT, USA Department of Pathology, University of Utah School of Medicine, Salt Lake City, UT, USA
Mary Anne Karren
Affiliation:
Utah Center for Genetic Discovery, Department of Human Genetics, University of Utah, Salt Lake City, UT, USA
Luca Brunelli
Affiliation:
Division of Neonatology, Department of Pediatrics, University of Utah School of Medicine, Salt Lake City, UT, USA
Mark Yandell
Affiliation:
Utah Center for Genetic Discovery, Department of Human Genetics, University of Utah, Salt Lake City, UT, USA
Martin Tristani-Firouzi
Affiliation:
Division of Cardiology, Department of Pediatrics, University of Utah School of Medicine, Salt Lake City, UT, USA
David Dimmock
Affiliation:
Rady Children’s Institute for Genomic Medicine, San Diego, CA, USA
Brian Watts
Affiliation:
Office of General Counsel, University of Utah, Salt Lake City, UT, USA
Jeffrey R. Botkin
Affiliation:
Division of Medical Ethics, Department of Pediatrics, University of Utah, Salt Lake City, UT, USA
Ann Johnson
Affiliation:
Institutional Review Board, University of Utah, Salt Lake City, UT, USA College of Nursing, University of Utah, Salt Lake City, UT, USA
Joshua L. Bonkowsky*
Affiliation:
Division of Pediatric Neurology, Department of Pediatrics, University of Utah School of Medicine, Salt Lake City, UT, USA Primary Children’s Center for Personalized Medicine, Salt Lake City, UT, USA
*
Address for correspondence: J. Bonkowsky, MD, PhD, Department of Pediatrics, 295 Chipeta Way/Williams Building, Salt Lake City, UT84108, USA. Email: joshua.bonkowsky@hsc.utah.edu; S. Malone Jenkins, MD, Department of Pediatrics, 295 Chipeta Way/Williams Building, Salt Lake City, UT84108, USA. Email: Sabrina.MaloneJenkins@hsc.utah.edu
Address for correspondence: J. Bonkowsky, MD, PhD, Department of Pediatrics, 295 Chipeta Way/Williams Building, Salt Lake City, UT84108, USA. Email: joshua.bonkowsky@hsc.utah.edu; S. Malone Jenkins, MD, Department of Pediatrics, 295 Chipeta Way/Williams Building, Salt Lake City, UT84108, USA. Email: Sabrina.MaloneJenkins@hsc.utah.edu
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Abstract

Rapid whole genome sequencing (rapid WGS) is a powerful diagnostic tool that is becoming increasingly practical for widespread clinical use. However, protocols for its use are challenging to implement. A significant obstacle to clinical adoption is that laboratory certification requires an initial research development phase, which is constrained by regulations from returning results. Regulations preventing return of results have ethical implications in cases which might impact patient outcomes. Here, we describe our experience with the development of a rapid WGS research protocol, that balanced the requirements for laboratory-validated test development with the ethical needs of clinically relevant return of results.

Type
Brief Report
Information
Journal of Clinical and Translational Science , Volume 5 , Issue 1 , 2021 , e177
Creative Commons
Creative Common License - CCCreative Common License - BYCreative Common License - NCCreative Common License - ND
This is an Open Access article, distributed under the terms of the Creative Commons Attribution-NonCommercial-NoDerivatives licence (http://creativecommons.org/licenses/by-nc-nd/4.0/), which permits non-commercial re-use, distribution, and reproduction in any medium, provided the original work is unaltered and is properly cited. The written permission of Cambridge University Press must be obtained for commercial re-use or in order to create a derivative work.
Copyright
© The Author(s), 2021. Published by Cambridge University Press on behalf of The Association for Clinical and Translational Science

Introduction

Next-generation sequencing (NGS) technologies offer the potential to dramatically shorten diagnostic processes and improve clinical care [Reference Brunelli, Jenkins and Gudgeon1]. Rapid whole genome sequencing (rapid WGS) is a recent NGS advancement, providing results in a week or less. Advantages of rapid WGS include rapid turnaround and the ability to identify many different genetic variant types. Clinical use of rapid WGS has been of particular interest for infants in neonatal intensive care units (NICUs) where mortality rates can exceed 10% [Reference Horbar, Edwards and Greenberg2], and the median daily cost of patients can exceed $3,000 [Reference Apfeld, Kastenberg, Gibbons, Phibbs, Lee and Sylvester3]. Rapid WGS in the NICU has shown immediate as well as long-term benefits on infant health, outcomes, and costs [Reference Petrikin, Cakici and Clark4Reference Saunders, Miller and Soden8].

Currently, rapid WGS is available as a clinical test from only a few commercial laboratories in the USA. Recognizing this limitation, and the need for rapid WGS at our high acuity NICU, our goal was to develop and implement a rapid WGS test. However, our research development phase of rapid WGS required assessment of competing ethical issues and federal laws, that are recognized as contradictory, and that are likely to impact other centers across the country in their initial use of rapid WGS [Reference Milko, Chen and Chan9, 10]. Federal regulations for laboratory development of a new test require a research period prior to validation for clinical use, during which results are generated and precluded from return to patients and families. However, the research testing phase of rapid WGS raises an ethical challenge; namely, that results from rapid WGS could have immediately actionable findings. This brief report summarizes our center’s approach to development of rapid WGS, navigating research development, laboratory certification requirements, and ethical challenges.

Regulatory Considerations

This project (Utah NeoSeq) was approved by the University of Utah Institutional Review Board (IRB). The development of rapid WGS was a collaboration between the University of Utah Department of Pediatrics, the Utah Center for Genetic Discovery, and ARUP Laboratories, a large reference laboratory (Fig. 1).

Fig. 1. Regulation considerations during research rapid WGS (NeoSeq).

The NeoSeq consent contains language indicating HIPAA Right to Access and the parents’ request to receive research results. The patient has a clinical blood draw and sequencing is done under a research protocol at ARUP Laboratories which is a CLIA certified lab. Analysis is done at a separate non-CLIA facility by the Utah Center for Genetic Discovery. All results are returned to the family by the study and clinical teams and the benefits and risks of a change in management are discussed. This testing is done in parallel with normal standard of care testing. Abbreviations: CLIA, Clinical Laboratory Improvement Amendments; EMR, electronic medical records; FDA, Food and Drug Administration; HIPAA, Health Insurance Portability and Accountability Act of 1996; IDE, Investigational Device Examination; IRB, institutional review board; UCGD, Utah Center for Genetic Discovery.

Patient access to genomic research results is governed by a complex set of regulatory bodies and associated laws and standards [1013]. Initial discussions were in person between the study team and IRB committee. When the complex situation was recognized, we formed an expert panel of legal and ethical counsel, including members of the University of Utah IRB, University Office of General Counsel, bioethicists, genetic laboratory directors, and clinician researchers, with the goal of reviewing and evaluating applicable laws and weighing them with ethical considerations. We had a large in-person meeting then continued discussion by email. Here, we summarize the reviewed laws (Table 1) as they pertain to return of genomic research results and discuss the application of these laws to our study protocols in the subsequent sections.

Table 1. Federal regulatory laws governing return of Genomic research results

Abbreviations: CLIA, Clinical Laboratory Improvement Amendments; FDA, Food and Drug Administration; HIPAA, Health Insurance Portability and Accountability Act of 1996; IRB, institutional review board; SACHRP, Secretary’s Advisory Committee on Human Research Protections.

Bioethical Principles and Return of Results

Ethical considerations for implementing WGS in the NICU [Reference Lantos14, Reference Bell15] were a further consideration, given that as a research protocol there were competing interests of research result validity evaluation, and intervening in clinical care as quickly as possible. Although both interests strive to adhere to principles of benefice, nonmaleficence, and autonomy, they can be at practical and regulatory odds. For example, if there is a gene variant (pyridoxine-dependent epilepsy) that causes on-going seizures, for which there is a low-risk treatment, a research result may allow clinicians to discuss possible treatment with parents, allowing them to adhere to all three of the above principles. However, acting on an “uncertified” result could be countered to those same principles. Withholding possible treatment would also be unethical if doing so harmed the patient. If research WGS identified a relevant gene variant, it would be difficult to obscure the result from the family because of the need for confirmatory testing. This would also create the potential for distrust, as the healthcare team would be aware of the research finding but would be precluded from sharing this with the family. We balanced these competing interests by developing a plan to return results centered around shared-decision making [Reference Soltys, Philpott-Streiff, Fuzzell and Politi16].

CLIA Regulations

The Clinical Laboratory Improvement Amendments (CLIA) are federal regulatory standards that guide clinical laboratory testing of human specimens. CLIA standards do not apply to research testing if results are not reported for diagnosis, prevention, treatment, or other health assessment purposes [12]. Prior to use in clinical patient care, an expectation is that a laboratory research and validate any new test, such as rapid WGS.

Recognition of the Health Insurance Portability and Accountability Act (HIPAA) Right to Results

The norm for our institution’s informed consent process outlines a patient’s right to obtain their protected health information (PHI) including genetic test results from a designated record set (DRS) under the HIPAA privacy rule. As the rapid WGS is performed under a research protocol, we recognized that returning results prior to a CLIA-certified confirmation is in tension with CLIA regulations. In an effort to resolve the tension between HIPAA and CLIA on this point, some academic research institutions have developed policies to exclude research results from the DRS.

The National Academies of Sciences evaluated these conflicting and ambiguous regulatory laws governing the return of individual results [10]. Their recommendations included better defining the DRS and requiring all HIPAA-covered entities completing human biospecimen research to have an IRB-approved plan for the return of results when requested under HIPAA. However, these issues and recommendations remain unresolved by regulatory agencies.

We therefore included in the informed consent the discussion of the benefits and risks of using research results for clinical care, and that there might be an in-depth discussion on this topic at the time of return of results. For the study child, we report variants related to their clinical presentation. We also will report variants of uncertain significance if associated with their medical issues. We do not report variants of unknown significance (VUS) that are not related to the clinical presentation. For the family members, we will report the presence or absence of variants that are detected in the study child. Optional results for the study child and family members include the American College of Medical Genetics 59 medically actionable incidental findings, which we report if the family opts in. (see our informed consent in the Supplementary Information ). The results are returned to the family in person during a care conference by the study neonatologist, study medical geneticist, the attending neonatologist, and the attending medical geneticist. A research letter is also uploaded to the electronic medical record under the research tab. This allowed the research and clinical teams to utilize shared-decision making, whereby parents are engaged in NICU care decisions resulting in less decisional regret [Reference Soltys, Philpott-Streiff, Fuzzell and Politi16], with the goal to support parental autonomy and care provider obligation for beneficial care. The IRB would be contacted if there was a risk of harm to the patient from potential next steps guided by the research results.

Determination as a Nonsignificant Risk Device Study

Another important consideration was the determination that the proposed investigation would be considered a nonsignificant risk (NSR) device study. This requires approval of the protocol and compliance with NSR regulatory standards [17] but does not require submitting an Investigational Device Exemption (IDE) to the United States Food and Drug Administration (FDA).

This determination was based on a 2014 FDA decision regarding a comparable WGS study and the inclusion of appropriate risk-mitigating measures. In the 2014 precedent, the FDA had determined that the use of rapid WGS for critically ill neonates was a NSR study based on the following rationale: “1) Although you (the study) may return investigational test results to the treating physician that may influence important treatment decisions prior to their confirmation, this risk is lessened because the study population is critically ill, unlikely to be diagnosed quickly by other mechanisms, and suffers from a high mortality rate, 2) the treating physician can apply clinical judgment on whether treatment based on a preliminary, investigational result is warranted for a given patient, including considering the potential risk(s) the patient may incur given the nature/severity of the treatment, and 3) all returned investigational test results will ultimately be confirmed [Reference Litwack18].”

There were two other factors in the NSR determination. First, the research rapid WGS used existing certified personnel and processes; including the hospital, laboratory, and staff involved. Second, the return of results and any clinical care decisions were managed by a joint team of specialists, including medical geneticists and neonatologists.

The high accuracy of WGS technology was also taken into consideration. WGS has a well-demonstrated record of clinically appropriate sensitivity and specificity [Reference Shevchenko and Bale19], and the technology of Sanger sequencing used for CLIA confirmation is at a similar risk of errors as to WGS [Reference Strom, Lee and Das20Reference Mu, Lu, Chen, Li and Elliott22]. Therefore, rapid WGS technology itself was not a separate risk to consider for the study.

Discussion

NGS has the potential to transform care of critically ill infants in NICUs by providing early molecular diagnosis [Reference Willig, Petrikin and Smith5, Reference Saunders, Miller and Soden8, Reference Soden, Saunders and Willig23]. These benefits have accelerated efforts for clinical implementation of NGS such as rapid WGS. We describe a process that is of broad interest for the development of clinical rapid WGS, the balancing of laboratory certification requirements with ethical and HIPAA regulations. With advice from an expert panel of legal and ethical counsel, we created an IRB-approved protocol focused on informed consent, enabling clinical test validation to occur, in the setting of HIPAA right to access for families to ensure that medically actionable variants could be returned with the potential for clinical intervention.

The need for an approach to clinical development of rapid WGS arose because there are opposing regulations between laboratory testing validation requirements, HIPAA, and ethical considerations. Despite national committee recommendations [10], there are no accepted guidelines or regulations regarding the balance between the potential risks and errors of WGS completed in a research environment and the clinical need to act upon a rapid WGS result that may benefit a patient or significantly affect their outcome before results can be validated.

We concluded that honoring the HIPAA right to access PHI in the form of rapid WGS results was appropriate and ethically supported. The consensus of our expert panel was that withholding care in this situation would not be ethical. Considerations included sequencing being completed at a CLIA-certified laboratory, the goal of the research (evaluating outcomes of rapid WGS), careful phenotype-driven analysis, and level of stress and uncertainty the families already are under.

Although it is possible for a scenario to occur where a WGS result is uncertain, but clinical intervention is of immediate concern and would require CLIA-based sequencing confirmation, this scenario is unlikely to occur in a fashion to impact patient care. This is because of the technical robustness of WGS, along with the low rate of results requiring clinical intervention in a time frame that would preclude CLIA-based sequencing or other orthogonal measures to demonstrate the validity of the WGS result.

In summary, with our collaborative approach, we defined a protocol that balances research standards and process with the potential clinical utility of a result. Our approach honors the Centers for Medicare and Medicaid Services’ regulations governing CLIA certification of laboratory results before clinical intervention for the majority of nonurgent results. However, when the results are deemed critical for a prompt intervention by clinicians, our approach honors the right of parents under HIPAA to request results that are part of the DRS. This request is incorporated into the consent process. Continued research is needed in this area, including impacts on patients, families, and healthcare providers. We hope our described experience and research will provide a foundation for this process to be implemented at other institutions.

Supplementary Material

To view supplementary material for this article, please visit https://doi.org/10.1017/cts.2021.833.

Acknowledgements

This study is funded by the Center for Genomic Medicine at the University of Utah Health, ARUP Laboratories, Illumina, and the Margolis Foundation.

Disclosures

MY is a co-founder, scientific advisory board member, and consultant for Fabric Genomics Inc. JRB is a consultant to Sanofi Pharmaceuticals. DD reports previous consulting fees from Audentes, Biomarin, Ichorion, and Complete Genomics. He serves on a scientific advisory board for Taysha Gene Therapies. DD is an inventor on US patent 8718950B2 assigned to The HudsonAlpha Institute for Biotechnology. JLB has served as a consultant to Bluebird Bio, Inc; to Calico, Inc; to Denali; to Neurogene, Inc.; to Enzyvant, Inc.; to Passage Bio; and owns stock in Orchard Therapeutics. The remaining authors have no conflicts of interest to declare.

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Figure 0

Fig. 1. Regulation considerations during research rapid WGS (NeoSeq).The NeoSeq consent contains language indicating HIPAA Right to Access and the parents’ request to receive research results. The patient has a clinical blood draw and sequencing is done under a research protocol at ARUP Laboratories which is a CLIA certified lab. Analysis is done at a separate non-CLIA facility by the Utah Center for Genetic Discovery. All results are returned to the family by the study and clinical teams and the benefits and risks of a change in management are discussed. This testing is done in parallel with normal standard of care testing. Abbreviations: CLIA, Clinical Laboratory Improvement Amendments; EMR, electronic medical records; FDA, Food and Drug Administration; HIPAA, Health Insurance Portability and Accountability Act of 1996; IDE, Investigational Device Examination; IRB, institutional review board; UCGD, Utah Center for Genetic Discovery.

Figure 1

Table 1. Federal regulatory laws governing return of Genomic research results

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