eCase - 2022 WCLC Highlights

CME

Independent Conference Coverage of the IASLC 2022 World Conference on Lung Cancer

Physicians: Maximum of 1.00 AMA PRA Category 1 Credit™

Released: October 25, 2022

Expiration: October 24, 2023

Wade T. Iams, MD, MSCI

Heather Wakelee, MD

CME/CE Information

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Introduction Early-Stage NSCLC Advanced NSCLC With No Actionable Mutations Advanced NSCLC With Actionable Mutations SCLC Population-Based Assessments References

Second-Course Pembrolizumab: Background

Wade T. Iams, MD, MSCI:
Our current standard of care regimens for patients with advanced NSCLC without actionable biomarkers, such as EGFR or ALK alterations, includes immune checkpoint inhibitor therapy with or without chemotherapy. The duration of immune checkpoint inhibitor therapy varies; for example, you can stop pembrolizumab at 2 years based on the trials supporting the use of this agent. A recurring question in the clinic that patients invariably ask is, “What happens if my cancer grows after I stop pembrolizumab?”

This next study was a dataset compiled from patients with advanced NSCLC who received a second course of single-agent pembrolizumab after cessation in 5 prospective clinical trials.⁸I think this is a practical and important dataset to review.

Second-Course Pembrolizumab: Pooled Analysis Design

Wade T. Iams, MD, MSCI:
This exploratory analysis was a dataset compiled from patients with advanced NSCLC who received a second course of single-agent pembrolizumab after previous cessation in 5 prospective clinical trials.⁸These patients with stage IV nonsquamous or squamous NSCLC without EGFR/ALK mutations were eligible for a second course of pembrolizumab after either having previous stable disease or better with 35 cycles of first-course pembrolizumab or stopping first-course pembrolizumab after ≥8 cycles with a confirmed CR. Patients were divided into 2 cohorts: those with first-course pembrolizumab monotherapy (cohort 1, including patients from KEYNOTE-024, KEYNOTE-042, and KEYNOTE-598) or those with first-course pembrolizumab plus chemotherapy (cohort 2, including patients from KEYNOTE-189 and KEYNOTE-407).⁸

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Second-Course Pembrolizumab: Patient Disposition

Wade T. Iams, MD, MSCI:
In cohort 1, approximately 5% of patients (57 total) received second-course pembrolizumab as a part of the clinical trial protocol. In cohort 2, approximately 2% of patients (14 total) received second-course pembrolizumab.⁸

From these data, you can see that there is a low percentage of patients who received a second-course pembrolizumab. In clinical practice, I provide a lot of reassurance for my patients when they are stopping pembrolizumab; I tell them that there is a very low risk that they will have tumor growth. With this dataset, we now also have data on efficacy when you retreat with pembrolizumab.

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Second-Course Pembrolizumab: BL Characteristics at Randomization of Initial Study

Wade T. Iams, MD, MSCI:
The baseline characteristics of patients who received pembrolizumab monotherapy or pembrolizumab plus chemotherapy on the KEYNOTE trials and then received a second course of pembrolizumab are similar.⁸ As we look ahead to the results from this analysis, it is important to remember that a higher proportion of patients who received first-course pembrolizumab monotherapy had a PD-L1 tumor proportion score (TPS) score ≥50% vs those who received combination therapy (81% vs 36%), which reflects current practice and does anticipate some of the results clinically.

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Second-Course Pembrolizumab: Survival and Tumor Response

Wade T. Iams, MD, MSCI:
When assessing the efficacy of a second course of pembrolizumab, the disease control rate is important to understand if retreatment with pembrolizumab is able to regain control the cancer. The disease control rate with pembrolizumab retreatment was 74% for patients who received first-line pembrolizumab monotherapy and 50% in patients who received pembrolizumab plus chemotherapy initially.⁸

In an analysis of the objective response rate (ORR) with pembrolizumab retreatment by PD‑L1 expression in cohort 1 (first-line pembrolizumab monotherapy), the ORR for the overall population was 19.3%, 17.4% for patients with PD-L1 TPS ≥50%, and 27.3% for patients with a PD-L1 TPS of 1% to 49%. The CIs were large, especially for the PD‑L1 1% to 49% group, so it is difficult to interpret these data with certainty.

The median DoR with pembrolizumab retreatment was not reached at data cutoff, but the 6-month DoR rate was 79%. The median PFS with pembrolizumab retreatment was 10.3 months after previous pembrolizumab monotherapy and 7.7 months after pembrolizumab plus chemotherapy. The median OS with pembrolizumab retreatment was 27.5 months after previous pembrolizumab monotherapy and not yet reached after pembrolizumab plus chemotherapy.

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Second-Course Pembrolizumab: Duration of Response in Cohort 1 Individual Patients

Wade T. Iams, MD, MSCI:
This swimmers plot for cohort 1 depicts the treatment course of patients who received first-course pembrolizumab monotherapy, the time of PD, and subsequent treatment and response to second-course pembrolizumab. The median time from stopping first-course pembrolizumab monotherapy to retreatment with second-course pembrolizumab was 12 months.⁸ In this small cohort of patients who received pembrolizumab retreatment after a course of pembrolizumab monotherapy, it was approximately 1 year from stopping their first-course pembrolizumab to second-course initiation, which is important clinical context when counselling patients about pembrolizumab cessation.

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Second-Course Pembrolizumab: Duration of Response in Cohort 2 Individual Patients

Wade T. Iams, MD, MSCI:
In cohort 2 with patients who received first-course pembrolizumab plus chemotherapy initially, the median time from stopping first-course pembrolizumab to second-course initiation was a little shorter at 5.4 months.⁸ This was an even smaller group, with only 14 patients, so it is difficult to make broad statements about these data.

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Second-Course Pembrolizumab: Safety

Wade T. Iams, MD, MSCI:
The safety profile is an important component of this study as well. The types of adverse events that were observed with second-course pembrolizumab were aligned with what we generally see with pembrolizumab in our patients with NSCLC, including thyroid-related and dermatologic adverse events.⁸

There were no surprising safety signals and pembrolizumab retreatment seems like a manageable option for patients.

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Second-Course Pembrolizumab: Conclusions

Wade T. Iams, MD, MSCI:
This pooled analysis of patients who received a second course of pembrolizumab as a part of 5 different clinical trials is an important dataset that can help inform discussions with patients in the clinic when completing a course of pembrolizumab at 2 years. We now know that a second-course pembrolizumab can be a good option to regain disease control in a majority of patients.

When we look at the efficacy data, it is important to consider additional context with second-course pembrolizumab as it relates to recent data from the Lung-MAP S1800A substudy presented at ASCO 2022. In this trial, patients previously treated with an immune checkpoint inhibitor and platinum-based chemotherapy who had progressive disease showed a similar objective response and PFS but improved OS with pembrolizumab plus ramucirumab compared with changing to a standard-of-care cytotoxic chemotherapy.⁹There appears to be a subset of patients who are still deriving benefit from immune checkpoint inhibitor therapy even after progression and this can result in durable survival results.

Heather Wakelee, MD:
This has been a critical clinical question. I had a patient in clinic yesterday with this exact scenario, where he was approaching 2 years on pembrolizumab therapy and we were questioning whether we should stop or continue pembrolizumab therapy. If pembrolizumab therapy is discontinued, what do you do next?

Cohort 1 consisted of patients from KEYNOTE-024, KEYNOTE-042, and KEYNOTE-598 who had a PD‑L1 TPS of ≥1% or ≥50%. In these trials, 1160 patients were enrolled to receive pembrolizumab monotherapy. Only 223 patients completed 35 cycles of pembrolizumab and 123 experienced progression after therapy was stopped. Cohort 2 consisted of patients from KEYNOTE-189 and KEYNOTE-407 regardless of PD‑L1 expression. In these 2 trials, 763 patients were enrolled to receive pembrolizumab plus chemotherapy. In this subset, 125 patients completed 35 cycles of pembrolizumab and 57 experienced progression after therapy was stopped.

This is one of the things I emphasize with my patients who approach 2 years of therapy with pembrolizumab: if we stop therapy, there is approximately a 50% chance the cancer is not going to return, but a 50% chance it could.

We do not know what happens if you continue pembrolizumab therapy beyond 2 years, but these data do suggest that restarting with a second course of pembrolizumab can help regain control of the disease.

Many of the patients from these trials have had a complete response to initial therapy or have minimal disease at progression, so it can be difficult to define a meaningful response. It is unclear whether a CR or PR is more meaningful than simply having the disease under control; however, the fact that a large percentage of these patients were able to see their disease back under control with pembrolizumab retreatment is great.

Now, we need to try to address the question of who should stay on pembrolizumab indefinitely and who can stop safely and know that restarting a second course of pembrolizumab can regain tumor control.

A 60-year-old woman with a smoking history was diagnosed with advanced NSCLC with 70% PD-L1 and next-generation sequencing (NGS) results positive for a KRAS G12V mutation. She began therapy with single-agent pembrolizumab, achieved a partial response (PR), and has completed 30 cycles. What can you tell her about the potential to resume pembrolizumab at disease progression once she completes 35 cycles of pembrolizumab?

A. There is approximately a 20% chance the cancer is not going to return after completing 35 cycles of single-agent pembrolizumab
B. The median time from stopping first-course pembrolizumab monotherapy to beginning a second course of pembrolizumab is 3 months
C. Approximately 75% of patients who received first-line pembrolizumab monotherapy experience disease control with pembrolizumab retreatment
D. Less than one half of patients who respond to a second course of pembrolizumab remain in response at 6 months

TROPION-Lung02: Background

Heather Wakelee, MD:
So far, we have discussed immune checkpoint inhibitor–based treatment options for patients with NSCLC and no actionable genomic alterations. Although treatment with an immune checkpoint inhibitor with or without chemotherapy has improved outcomes for these patients, disease progression does occur and treatment options become more limited.

TROP2 is a transmembrane glycoprotein associated with poor prognosis in NSCLC.¹⁰Datopotamab deruxtecan (Dato-DXd) is an antibody–drug conjugate (ADC) with a humanized anti‑TROP2 antibody linked to a topoisomerase I inhibitor payload, and it has had some earlier data showing encouraging activity in advanced NSCLC.¹¹

TROPION-Lung02: Study Design

Heather Wakelee, MD:
TROPION-Lung02 is a phase Ib study that is assessing various combinations with Dato-DXd, including as a doublet with pembrolizumab or a triplet with pembrolizumab and carboplatin or pembrolizumab and cisplatin in patients with advanced NSCLC without actionable genomic alterations. In the dose confirmation phase, patients could have received ≤2 previous lines of therapy and in the dose expansion phase, patients assigned to doublet therapy could have received ≤1 previous lines of platinum-based therapy, whereas patients assigned to triplet combinations received no previous therapy.¹²

The primary endpoint was safety and tolerability and the secondary endpoints included efficacy, pharmacokinetics, and presence or absence of antidrug antibodies.

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TROPION-Lung02: Baseline Characteristics and Treatment Disposition

Heather Wakelee, MD:
This trial enrolled 40 patients in the doublet cohorts and 48 patients in the triplet cohorts at the time of this analysis.

Most patients were men (70%) and had nonsquamous histology (70%-85%). In the doublet cohorts, the median number of previous lines of therapy was 1 and 33% received Dato-DXd and pembrolizumab as their first line of therapy. In the triplet cohorts, the median previous lines of therapy was 0 and 63% received Dato-DXd and pembrolizumab plus a platinum agent as their first line of therapy.¹²

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TROPION-Lung02: Safety

Heather Wakelee, MD:
Study treatment–related grade ≥3 treatment‑emergent adverse events were reported in 35% of patients receiving Dato-DXd and pembrolizumab and 54% of patients receiving Dato-DXd and pembrolizumab plus a platinum agent.¹² Since these patients were receiving various treatments in combination, these numbers are not unexpected.

Drug‑related pneumonitis or interstitial lung disease is something healthcare professionals need to be mindful of with any ADC. In this trial, drug-related interstitial lung disease was reported in 8% of patients receiving Dato-DXd and pembrolizumab (3% were grade 3) and 2% of patients receiving Dato-DXd and pembrolizumab plus a platinum agent (all grade 3). Stomatitis also occurred in 48% of patients receiving doublet therapy and 23% of patients receiving triplet therapy, and this is not something often reported with pembrolizumab plus platinum therapy. Other adverse events were as expected.

There were 3 deaths on the trial (5% of patients receiving doublet therapy and 2% of patients receiving triplet therapy) but these were advanced‑stage patients, and most were not believed to be drug related.

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TROPION-Lung02: Efficacy

Heather Wakelee, MD:
The response rate was 37% in patients receiving Dato-DXd and pembrolizumab, and it was 41% in patients receiving Dato-DXd and pembrolizumab plus a platinum agent. With small numbers in each cohort, it is not clear if these numbers are meaningfully different. Overall, 84% of patients achieved disease control in each cohort.¹²

For patients who received therapy as first-line treatment, the response rate was 62% with the doublet and 50% with the triplet. In addition, 39% of patients receiving Dato-DXd and pembrolizumab and 40% receiving Dato-DXd and pembrolizumab plus a platinum agent achieved stable disease, making the disease control rate 100% and 90%, respectively.¹²

In the second-line population, intriguingly enough, the response rate for Dato-DXd and pembrolizumab was 24% and was 29% with Dato-DXd and pembrolizumab plus a platinum agent.¹²

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TROPION-Lung02: Conclusions

Heather Wakelee, MD:
Overall, these data suggest that there is some advantage to combining the TROP2 ADC, Dato-DXd, with immune checkpoint inhibitor therapy with or without chemotherapy. The doublet with Dato-DXd and pembrolizumab resulted in response rates that were somewhat higher than you would expect with pembrolizumab alone in first-line and second-line metastatic NSCLC. When you add a platinum agent along with Dato-DXd and pembrolizumab, there is added toxicity and it is not clear if it significantly improves response rates. This may be a reasonable strategy to consider, but more data are needed to confirm these results.

In general, we consider ADCs to be a new class of therapy, but they are basically using antibodies for target delivery of some of our standard chemotherapeutic modalities. One question is whether the substitution of an ADC in place of one of our standard chemotherapies, such as a taxane or pemetrexed, is making a big leap forward for patient outcomes. At this point, it is not clear, but there are a few phase III trials currently recruiting to help answer some of these questions. For example, the TROPION-Lung08 trial will compare Dato‑DXd plus pembrolizumab vs pembrolizumab alone as first‑line therapy for patients with metastatic NSCLC who have high PD‑L1 expression (TPS ≥50%). The TROPION-Lung07 trial will compare Dato‑DXd plus pembrolizumab vs Dato-DXd plus pembrolizumab plus platinum chemotherapy vs pembrolizumab plus pemetrexed plus platinum chemotherapy for patients with metastatic NSCLC who have a PD‑L1 TPS <50%. I think these are reasonable studies to ask the question of whether adding a single‑agent chemotherapy with an ADC to pembrolizumab can make a meaningful impact on patient outcomes.

Wade T. Iams, MD, MSCI:
I agree, this is not yet practice changing, but these data do warrant further evaluation and I am most interested to see additional results with the Dato‑DXd plus pembrolizumab doublet. When having a conversation with a patient, the discussion often centers around the tradeoff between the likelihood of durable disease control compared with the potential for toxicity. The adverse events associated with Dato-DXd is not negligible, so it is important to be cognizant of this when deciding on treatment approaches and to consider whether we see enough of an improvement in durable disease control to warrant additional potential toxicity.

HUDSON: Background

Wade T. Iams, MD, MSCI:
In addition to exploring new treatment options for patients with advanced NSCLC whose disease has progressed on or after immune checkpoint inhibitor therapy, other studies are trying to address mechanisms of resistance to PD‑1 or PD‑L1 inhibitors by evaluating potential drivers of resistance and treatment options that can exploit these drivers.

The HUDSON trial is a phase II umbrella study that used molecular screening to match patients with various potential driver mutations to targeted therapy combinations. Cohorts include those that are biomarker matched (eg, patients with ATM mutations who received the ATR inhibitor ceralasertib in combination with durvalumab) and those that were not matched.

The mechanisms that were assessed included those that target the DNA damage repair pathways, such as ATM mutations and homologous recombination as well as HER2 expression or mutations. The most successful approach to date was the use of the ATR inhibitor ceralasertib, particularly among patients with ATM mutations. Other strategies that were evaluated used a PARP inhibitor, olaparib; an epigenetic modifier STAT3 inhibitor, danvatirsen; an anti‑CD73 monoclonal antibody, oleclumab; and the HER2-targeted ADC trastuzumab deruxtecan. Since ceralasertib is being further evaluated in subsequent trials, we will focus on these results in our discussion.

HUDSON: Study Design

Wade T. Iams, MD, MSCI:
As mentioned, HUDSON is a phase II umbrella trial that enrolled patients with advanced NSCLC with no EGFR, ALK, ROS1, BRAF, MET, or RET targetable mutations who had previously received platinum doublet therapy and a PD‑1 or PD‑L1 immune checkpoint inhibitor therapy. Patients were assigned to biomarker matched or nonmatched groups to receive durvalumab plus a targeted agent.

Patients who were biomarker matched (group A) included those with homologous recombination repair mutations and received durvalumab plus olaparib; with LKB1 aberrations and received durvalumab plus olaparib; with ATM mutations and received durvalumab plus ceralasertib or ceralasertib alone; were CD73^high and received durvalumab plus oleclumab; or with HER2 expression or mutations and received durvalumab plus trastuzumab deruxtecan.

Patients who were not matched by a specific biomarker (group B) were divided into those with primary resistance or acquired resistance (progression ≤24 or >24 weeks, respectively) and received durvalumab in combination with olaparib, danvatirsen, ceralasertib, oleclumab, or cediranib.

The primary endpoint was ORR and secondary endpoints included disease control rate, PFS, and safety.¹³

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HUDSON: Baseline Characteristics by Treatment (Groups A and B)

Wade T. Iams, MD, MSCI:
The baseline characteristics were pretty well matched among different cohorts. The median age was approximately 65 years and a little more than one half were men. Most had adenocarcinoma, and between 25% and 55% were PD-L1 positive. There was a moderate number of patients in each cohort ranging from 45 to 87 patients.¹³

Each subgroup had a fair number of patients for making some conclusions.

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HUDSON: Efficacy by Treatment (Groups A and B)

Wade T. Iams, MD, MSCI:
When we look at the clinical outcomes with combined subgroups, ceralasertib (the ATR inhibitor) was particularly beneficial. Patients who received durvalumab plus ceralasertib reported an ORR of 16.7% and disease control at 12 weeks in 60% of patients and at 24 weeks in 42% of patients. Although these response data are not practice changing, the key takeaway is the contrast with the addition of olaparib (a PARP inhibitor), danvatirsen (a STAT3 inhibitor), or oleclumab (an anti‑CD73 antibody) to durvalumab. There were very few responses and no significant disease control in any of the other groups. The authors noted that because of this low response activity with durvalumab plus olaparib, danvatirsen, or oleclumab, these 3 regimens were pooled as an internal control.¹³

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HUDSON: PFS by Treatment (Groups A and B)

Wade T. Iams, MD, MSCI:
Similarly, the median PFS and the 6‑month PFS rate was better with ceralasertib plus durvalumab vs the other regimens. The median PFS with ceralasertib plus durvalumab was 6 months and the 6‑month PFS rate was 46.3%.¹³

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HUDSON: OS by Treatment (Groups A and B)

Wade T. Iams, MD, MSCI:
Again, the median OS and the 12‑month OS rate was better with ceralasertib plus durvalumab vs the other regimens. The median OS with ceralasertib plus durvalumab was 15.9 months and the 12‑month PFS rate was 61.6%.¹³

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HUDSON: Efficacy by Cohort (Durvalumab Plus Ceralasertib)

Wade T. Iams, MD, MSCI:
In the biomarker‑matched cohort of patients with an ATM mutation who received ceralasertib plus durvalumab, there was a clear enrichment in clinical benefit vs nonmatched patients with either primary or acquired resistance who received ceralasertib plus durvalumab. These data suggest that ATM mutations can predict the efficacy of ceralasertib when combined with durvalumab. These are intriguing data, but the cohorts of patients were small, so I think it still has to be further evaluated.

In the 21 patients who were biomarker matched with an ATM mutation, the ORR was 29%, the median PFS was 8.4 months, and the median OS was 22.8 months. In the patients who were nonmatched with primary resistance (n = 20) or acquired resistance (n = 25), the ORR was 15% and 8%, the median PFS was 4.9 months and 4.6 months, and the median OS was 11.8 months and 19.1 months, respectively.¹³

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HUDSON: Safety by Treatment (Groups A and B)

Wade T. Iams, MD, MSCI:
In terms of safety, we should be very cognizant of the potential clinical benefit vs the potential for added adverse events with combination therapy and considering whether biomarkers can help select for patients who have the highest probability of having benefit.

For patients who received durvalumab plus ceralasertib, there was a moderate-to-large amount of grade ≥3 treatment‑emergent adverse events (50% of patients treated with ceralasertib plus durvalumab). Treatment‑emergent adverse events resulted in discontinuation in 12% of patients and, unfortunately, 2 patients (3%) experienced treatment‑emergent adverse events resulting in death.

The most common (≥20%) treatment-related adverse events included nausea, vomiting, decreased appetite, and anemia with this combination.¹³

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HUDSON: Conclusions

Wade T. Iams, MD, MSCI:
The HUDSON trial was a well-designed umbrella study that aimed to test various potential mechanistic strategies to address acquired resistance to PD‑1/PD-L1 checkpoint inhibitors, both in a biomarker-informed and biomarker-agnostic fashion. The key cohort that emerged from this study was the cohort of patients treated with durvalumab plus the ATR inhibitor ceralasertib, particularly the improved clinical efficacy among patients with ATM mutations.

Heather Wakelee, MD:
I thought that was a great idea to do this type of umbrella trial to explore different agents that target mechanisms that are not specifically a driver but may be modifying other important targets in lung cancer. It was disappointing that we only had 1 strategy that has the potential to move forward, and even the data with the ceralasertib combination does not clearly have a positive risk–benefit profile. The ceralasertib combination is worth further exploration; however, there is a phase III trial planned to study that (LATIFY; NCT05450692). Perhaps of most importance, this trial can act as a framework for ways to assess other potential treatment strategies in the future.

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Users are expected to refrain from submitting comments or messages that are defamatory, hateful, or obscene or that harass others. Users may not impersonate any other person or violate any other person’s or entity’s legal rights or submit falsified credentials or experiences. Users agree that they will not submit any materials that violate or infringe any copyrights, trademarks, patents, trade secret, or other intellectual property rights of any third party. Clinical Education Alliance retains all copyrights in the content posted by users to its sites. Clinical Education Alliance may adopt additional rules to govern use of social media, message boards or forums, to which users will be subject.

Copyright and Other Legal Violations

If you believe that any material on this Web site infringes your copyright, please notify us as follows, under the Digital Millennium Copyright Act (“DMCA”). To notify us, the DMCA requires that you: 1. Send an email notice to Clinical Education Alliance at customersupport@clinicaloptions.com. 2. Include the following information in your email: a. Identify the copyrighted work(s) you claim is infringed; b. Identify the material you claim is infringing the copyright(s) and give enough information for Clinical Education Alliance to locate that material; c. Include a physical or electronic signature of the copyright owner or a person authorized to act on the copyright owner’s behalf (the “Claimant”); d. Include the Claimant’s name, address, and telephone number(s); e. Include a statement that the Claimant has a good faith belief that use of the disputed material is not authorized by the copyright owner or his agent; and f. Include a statement, under penalty of perjury, that the information in the notification of copyright infringement is accurate and that the Claimant is the copyright owner or is authorized to act on behalf of the copyright owner.

If you believe any content or material on the Clinical Education Alliance Sites violates any laws, please notify customersupport@clinicaloptions.com. Please include details about your concerns and an email address for contacting you.

Governing Law

Clinical Education Alliance controls the Clinical Education Alliance Sites from its offices in the state of Virginia in the United States of America. The Clinical Education Alliance Sites can be accessed from any of the United States and from other countries worldwide. Since the laws of each state or country may differ, both you and Clinical Education Alliance agree that the laws of Virginia, without regard to conflicts of laws principles, will apply to all matters relating to use of the Clinical Education Alliance Sites and materials, including software and applications.

Clinical Education Alliance makes no representation that materials on these sites are appropriate or available for use in countries aside from the United States. Accessing the Clinical Education Alliance Sites from territories where their contents are illegal is prohibited. Those who choose to access these sites from other locations do so at their own risk and are responsible for compliance with any and all applicable local laws or regulations.

Acceptance Procedure

By downloading or accessing materials on the Clinical Education Alliance Sites and/or directly from iTunes or registering with us, you agree to all the terms and conditions in this agreement, including the Terms of Use and Privacy Policy. If you disagree with any of these Terms of Use or Privacy Policy, please refrain from using the Clinical Education Alliance Sites or materials.

Privacy Policy

Because we provide education for healthcare professionals, we pay special attention to privacy issues. The purpose of our Privacy Policy is to identify the information we may collect about you, describe the uses we may make of your information and the security measures we take to protect it, and discuss your options for controlling your information. You can review our Privacy Policy by clicking on the “Privacy Policy” link at the bottom of designated pages on the Clinical Education Alliance Sites.

Disputes

If you fail to comply with these terms, we have the right to suspend or eliminate your account and remove any information you have placed on our site, including your registration information. We may also take any legal action we think is appropriate. If there is any dispute between us concerning this agreement or your use of any Clinical Education Alliance Site or materials or applications, we both agree to submit the dispute to nonbinding mediation, followed by binding arbitration. Both the mediation and the arbitration will be governed under the rules of the American Arbitration Association, and the venue for the arbitration will be Virginia.

Questions or Concerns About Our Terms of Use

For questions or concerns about these Terms of Use, please send an email to customersupport@clinicaloptions.com

These terms of use were last updated in July 2021.