Our Product and Pipeline

OLINVYK ® (oliceridine) injection

Oliceridine Injection

OliceridineOLINVYK is a G-protein biased MOR ligand in development for the management of moderate-to-severe acute painthat we are commercializing in hospitals or other controlled clinical settings where IVfor acute pain in adults that is severe enough to require an intravenous opioid therapy is warranted.analgesic and for whom alternative treatments are inadequate. It is an NCE with a novel mechanism of action at the MOR that enables more selective targetingaction.

vomiting, and constipation, which can be exacerbated by accumulation of active metabolites and by reduced renal clearance in patients with impaired kidney function. Currently availableThese shortcomings of conventional IV opioid options offer either fast onset with short duration of action (e.g. IV fentanyl), or slower onset with longer duration (e.g. IV morphine). These pharmacokinetic and pharmacodynamic, or PK/PD, profilesopioids create some practicalsubstantial challenges for healthcare providers in certain clinical practice situations.

Injectable non‑opioidnon-opioid analgesics are often used together with IV opioids in multimodal protocols for post‑surgicalpost-surgical pain management; however,management. However, these drugs, such as IV non‑steroidal anti‑inflammatorynon-steroidal anti-inflammatory drugs, or NSAIDs, IV acetaminophen, or local anesthetics such as bupivacaine, have their own potential for cardiovascular, hepatic and gastrointestinal side effects. In addition, none of these non‑opioid analgesic approachesnon-opioid analgesics offers great enoughsufficient efficacy to manage severe acute pain as a monotherapy in many patients.

We believe that there remainsOLINVYK addresses a significant unmet need for a highly effective IV opioid analgesic agent with an improveda differentiated safety, tolerability, and/orand PK/PD profile.

Clinical development

We are developing oliceridine for the management OLINVYK delivers IV opioid efficacy with a rapid 1-3 minute median onset of moderate‑to‑severe acute pain in hospitals or other controlled clinical settings where IV administration is warranted. In the future, we also may explore other formulations, such as transmucosal administration for breakthrough pain in additional, separate clinical trials.

Below is a summary of the clinical development work undertaken for oliceridine.

ATHENA Phase 3 Open Label Safety Study

We conducted a Phase 3, open label, multicenter study evaluating the safetyaction and tolerability of oliceridinerequires no dosage adjustments in patients with moderate-to-severe pain causedrenal impairment, a large patient population with significant medical complications.

OLINVYK was approved by surgery or medical conditions. The trial was designed to model real-world use, including the use of multi-modal analgesia. Patients were treated with oliceridine on an as-needed basis via IVFDA in August 2020 for both bolus and patient-controlled analgesia, or PCA, or both, as determined bydelivery and we initiated commercial launch of OLINVYK in the investigator.first quarter of 2021. The primary objective was to assess the safety and tolerability of oliceridine. Pain intensity was measuredDEA has classified oliceridine as a secondary endpoint.Schedule II controlled substance. Like other opioids, the label for OLINVYK contains a “boxed” warning and important safety information. Please consult www.olinvyk.com to view the prescribing information together with important safety information and boxed warning.

In the ATHENA study, 768 patients were treated with oliceridine. The most common procedures were orthopedic, gynecologic, colorectal, and general surgeries. Patients at elevated risk of opioid-related adverse events were well represented; more than 30% of patients were 65 years or older, and approximately 50% of patients were obese, with body mass index (BMI) >30 kg/m2. Only 2% of patients discontinued for adverse events, and 4% of patients discontinued for lack of efficacy. The most common adverse events were nausea, constipation, and vomiting. Adverse event rates associated with oliceridine administered by PCA and as-needed bolus dosing were similar, supporting the potential use of oliceridine in both administration paradigms.OLINVYK clinical data

APOLLO 1 and APOLLO 2 Phase 3 Studies

We conducted two pivotal efficacy trials evaluating oliceridineOLINVYK in patients with moderate-to-severe acute pain: the APOLLO 1 study, which evaluated pain for 48 hours following bunionectomy, and the APOLLO 2 study, which evaluated pain for 24 hours following abdominoplasty. In February 2017, we announced positive top line results from the APOLLO 1 and APOLLO 2 studies. In both studies, all dose regimens achieved the primary endpoint of statistically greater analgesic efficacy than placebo, as measured by responder rate. On the secondary endpoint of summary of pain intensity difference (SPID) assessed by numerical rating scale, in the APOLLO 1 study, all dose regimens achieved statistically greater pain relief compared to placebo, while in the APOLLO 2 study, the 0.35mg and 0.5mg dose regimens achieved statistically greater pain relief compared to placebo.

The APOLLO 1 and APOLLO 2 studies were both Phase 3, multicenter, randomized, double-blind, placebo- and active-controlled studies of oliceridine.OLINVYK. During the study period, a loading dose of placebo, morphine (4 mg), or oliceridineOLINVYK (1.5 mg) was administered first, and then patients used a PCA button to dose themselves as often as every 6 minutes with the same study drug: placebo, 1 mg morphine, or 0.1 mg, 0.35 mg, or 0.5 mg oliceridine.OLINVYK. If PCA dosing was inadequate to control pain, patients could request supplemental study medication (2 mg morphine or 0.75 mg oliceridine,OLINVYK, no more than once an hour). If the study medication regimen did not adequately manage pain, patients could opt for an NSAID rescue analgesic. Loading, demand, and supplemental doses were volume-matched for all treatment regimens.

All endpoints were the same in both studies, except that dosing and pain assessment were for 48 hours in APOLLO 1 and 24 hours in APOLLO 2. EfficacyThe primary efficacy outcome was measured byusing a categorical responder analysis, which defined a responder as a patient who experienced at least a 30% reduction in their sum of pain intensity difference at the end of the treatment period without either early discontinuation (for lack of efficacy or safety/tolerability) or use of rescue medication. The summary of pain intensity difference (SPID), which the FDA used as the basis of approval, was a secondary endpoint in both studies and was assessed by numerical rating scale through

In both studies, oliceridineOLINVYK was generally well-tolerated. The most common drug related adverse events (incidence ≥10%) were nausea, vomiting, dizziness, headache, constipation, pruritus and dizziness.hypoxia.

ATHENA Phase 2b trial of oliceridine in acute postoperative pain following abdominoplasty3 Open Label Safety Study

The aim of ourWe conducted a Phase 2b clinical trial was to evaluate3, open label, multicenter study evaluating the efficacy, safety and tolerability of oliceridineOLINVYK in the management of postoperative pain using morphine as a benchmark, utilizing on demand dosing to reflect standard clinical practice. This Phase 2b trial was a randomized, double blind, placebo and active controlled trial of oliceridine in which we enrolled 200 patients with moderate-to-severe acute postoperative pain after abdominoplasty surgery. Two regimens of oliceridine were tested: the first consisted of a 1.5 mg intravenous loading dose with 0.1 mg self-administered on demand doses as often as every six minutes using a PCA device; the second consisted of a 1.5 mg loading dose with 0.35 mg on demand doses as often as every six minutes using a PCA device. A commonly used morphine PCA regimen also was tested, consisting of a 4 mg loading dose with 1 mg on demand doses as often as every six minutes. Placebo was administered as a loading dose and on demand doses were volume matched to the active regimens. Rescue medication consisting of ibuprofencaused by surgery or oxycodone was used in all groups.

In August 2015, we reported top line results from this trial. Oliceridine demonstrated statistically significant pain reduction compared to placebo and comparable efficacy to morphine. Oliceridine provided rapid reduction in average pain scores, consistent with the previous Phase 2 trial where oliceridine showed more rapid onset of meaningful pain relief than morphine. Rescue analgesic use was similar for both oliceridine and morphine, and less than half the rate of rescue analgesic use for placebo. In this study, the oliceridine groups had a significantly lower incidence (percentage of patients) of hypoventilation events (a measure of respiratory safety), nausea, and vomiting than the morphine group.medical conditions. The most frequently reported adverse events, associated with oliceridine were nausea, vomiting, hypoventilation and headache. Opioid related adverse events were generally less frequent in the oliceridine groups compared to morphine. No drug related serious adverse events were reported in the study.

Phase 2a/b trial of oliceridine in acute postoperative pain following bunionectomy

The aim of our Phase 2a/b clinical trial was designed to evaluatemodel real-world use, including the efficacyuse of multi-modal analgesia. Patients were treated with OLINVYK on an as-needed basis via IV bolus, patient-controlled analgesia, or PCA, or both, as determined by the investigator. The primary objective was to assess the safety and tolerability of oliceridine in the management of postoperative pain using morphine as a benchmark, using fixed dose and dose interval to characterize the performance of oliceridine. The trial was a multicenter, randomized, double blind, placebo and active controlled, multiple dose, adaptive trial in 333 women and men undergoing a primary unilateral first metatarsal bunionectomy surgery at four sites in the United States. Patients were randomized after surgery to receive oliceridine, morphine or placebo to manage their pain.OLINVYK. Pain intensity was measured using validated numeric rating scales ranging from ten (most severe pain)as a secondary endpoint.

In the ATHENA study, 768 patients were treated with OLINVYK. The most common procedures were orthopedic, gynecologic, colorectal, and general surgeries. Patients at elevated risk of opioid-related adverse events were well represented; more than 30% of patients were 65 years or older, and approximately 50% of patients were obese, with body mass index (BMI) >30 kg/m2. Only 2% of patients discontinued for adverse events, and 4% of patients discontinued for lack of efficacy. The most common adverse events were nausea, constipation, and vomiting. Adverse event rates associated with OLINVYK administered by PCA and as-needed bolus dosing were similar, supporting the potential use of OLINVYK in both administration paradigms.

OLINVYK Post-Approval Studies

Safety Differentiation Study. In May 2021, we announced an open-label, multi-site clinical trial to zero (no pain) at multiple time points up to 48 hours. Basedfurther characterize the impact of OLINVYK on these scales, analgesic efficacy was assessed with a time weighted average change in pain score over 48 hours—a well-established measure of changesrespiratory, gastrointestinal, or GI, and cognitive function outcomes in the intensity of pain over timepostoperative setting. The study, which will enroll approximately 200 adults undergoing major surgery, is led by clinical outcomes research experts from Cleveland Clinic and an FDA recommended endpoint for pain studies.

In November 2014, we announced top lineWake Forest Baptist Health. Respiratory safety will be assessed by continuous monitoring. Additional outcomes will include GI tolerability as measured by GI complete response, and cognitive function as measured by standardized somnolence, sedation, and delirium assessment scales. We expect to report topline data from this trial. At dosesstudy during the second half of 2 mg2022.

Respiratory Physiology Study. In July 2021, we announced a study evaluating the physiologic impact of OLINVYK on respiratory function in elderly and 3 mg of oliceridine administered every three hours, theobese subjects. This is a randomized, double-blind, four-period crossover trial achieved its primary endpoint of statistically greater pain reduction than placebo for 48 hours, which we believe demonstrated proof-of-concept for oliceridine. Over the 48-hour trial period, the 3 mg dose of oliceridine administered every three hours also showed statistically superior analgesic efficacy compared to the 4 mg dose of morphine administered every four hours. Additionally, in the first three hours of dosing, when pain was most severe, the 1 mg, 2 mg, and 3 mg doses of oliceridine demonstrated superior analgesic efficacy in the trial compared to placebo, 2 mg, and 3 mg doses of oliceridine demonstrated superior analgesic efficacy compared to the 4 mg dose of morphine.

There were no serious adverse events reported in the trial. Both the 2 mg and 3 mg doses of oliceridine showed overall tolerability over the 48-hour trial period similar to that of the 4 mg dose of morphine administered every four

hours. The most frequently reported adverse events associated with oliceridine were dizziness, headache, somnolence, nausea, vomiting, flushing and itching. Adverse effects were generally dose related.

Phase 1 clinical studies of oliceridine

We also have completed a number of Phase 1 clinical studies of oliceridine. These included two single ascending dose studies of oliceridine given as a 60-minute continuous infusion or a 2-minute bolus infusion that showed dose related increases in plasma exposure and pupil constriction, a biomarker for CNS opioid activityenrolling approximately 15 subjects ≥ 55 years old across a range of BMIs. All subjects will receive two doses of OLINVYK and two doses of IV morphine to obtain a range of plasma concentrations that were generally well tolerated.

In 2013, we completedspan the clinically relevant range for each medication. Respiratory depression will be assessed using the ventilatory response to hypercapnia, or VRH, measure, which is widely recognized as a Phase 1b proof-of-concept exploratory trialprecise method to assess respiratory physiology in healthy male subjects.humans. Analgesia will be measured using electrical stimulation of the anterior tibial surface, which is a valid and sensitive index of the pharmacologic effects of opioid agonists. The aims of this trial were to characterize the analgesic efficacy and safety and tolerability of a single dose of oliceridine as compared to a single 10 mg dose of morphine. We used a well-established evoked pain model, the cold pain test, tostudy will evaluate the ventilatory and analgesic effects of oliceridine by measuring the time to hand removal, or latency, from a temperature controlled cold water bath. At both the 3.0 mg and 4.5 mg doses, oliceridine showed superior efficacy as compared to a 10 mg morphine dose that was statistically significant with a p value of less than 0.05 at the ten- and thirty-minute time points after dosing. The durability of the analgesic effect was similar to morphine. In addition, the time to peak effect was more rapid than that for morphine. Overall, oliceridine was well tolerated in the trial. Subjects receiving oliceridine showed less severe nausea and less frequent vomiting at the 1.5 mg and 3.0 mg doses as compared to a 10 mg dose of morphine. Oliceridine also showed less respiratory depression compared to morphine over 4 hours.

In October 2014 we completed an adaptive, multiple ascending dose study of oliceridine in more than 50 healthy subjects. The safety, tolerability, pharmacokinetic and pharmacodynamics results of this study were consistent with the early Phase 1 studies described above. We also successfully completed an absorption, distribution, metabolism, and excretion study, with results consistent with the lack of known active oliceridine metabolites. We also completed a single-dose thorough QT study, a renal impairment study which showed no evidence of altered PK/accumulation in patients with renal failure compared to healthy patients, and a human abuse liability study which showed that oliceridine had similar abuse liability as IV morphine when administered at a comparably analgesic dose. In addition, we have completed a study in patients with underlying hepatic impairment, which showed that less frequent oliceridine dosing may be required in patients with severe hepatic impairment.

Regulatory Background and NDA Submission

In late 2017, we submitted the NDA for oliceridine to the FDA and in November 2018, the FDA issued a CRL related to the NDA. In the CRL, the FDA requested additional clinical data on the QT interval and indicated that the submitted safety database was not of adequate size for the proposed labeling at a maximum daily dose of 40 mg. The FDA also requested certain additional nonclinical data and validation reports. In January 2019, we announced the receipt of the official Type A meeting minutes from the FDA regarding the CRL wherein the FDA agreed that the submitted safety database would support labeling at a maximum daily dose of 27 mg. The FDA also agreed that we could conduct a study in healthy volunteers to collect the requested QT interval data and that the study should include placebo- and positive-control arms. We submitted a detailed protocol and analysis plan to the FDA and received feedback from the FDA on key design elements for the study and analysis plan. To address remaining items in the CRL, the FDA indicated that we should include supporting nonclinical data related to the characterization of the 9662 metabolite and the remaining method validation report in our resubmission of the NDA for oliceridine. 

We began the healthy volunteer QT study in June 2019. This was a randomized, single-site, placebo- and positive-controlled three-period crossover study conducted in 68 healthy volunteers, with 59 subjects receiving the maximum daily dose of 27 mg of oliceridine. Subjects were randomly sequenced through all three study periods: IV oliceridine, placebo, and a single oral dose of 400 mg moxifloxacin as a positive control. For the oliceridine and placebo arms, 2 or 3 mg of oliceridine or volume-matched placebo were administered by IV bolus every two hours over a 24-hour period. Electrocardiograms for all subjects were obtained at hourly time points using continuous Holter monitoring.

treatments. We reported topline data from this study in the first quarter of 2022.

IV morphine to obtain a range of plasma concentrations that span the prior safety database. There were four study discontinuations,clinically relevant range for each medication. Cognitive function will be evaluated using tests contained within the NeuroCart® test battery, a validated neurocognitive test methodology. A broad array of cognitive outcomes will be evaluated including three for lackmotor performance, attention, reaction time, memory and executive function. Analgesia will be determined by assessment of venous access and one for a non-serious adverse event, an asymptomatic and transient occurrence of non-sustained ventricular tachycardia, or briefly accelerated heart rate, confounded by hypokalemia, or low potassium levels, with no associated QT prolongation. One subject also completed dosing but was not evaluable duepain thresholds using the cold pressor test. We expect to equipment malfunction. There were no serious adverse events in the study.

The primary endpoint was the placebo-corrected change from baseline in the individual rate-corrected QT interval, measured hourly at each of the 24 time points in the study. On this outcome, the mean increase in the QT interval was less than 10 milliseconds at 22 of the 24 time points. The peak mean increase in QT interval was observed at 9 hours and was 11.7 milliseconds, with a 90% two-sided confidence interval upper bound of 14.7 milliseconds at this time point. At 18 of the 24 measured time points, the upper bound of the 90% confidence intervals for the mean increase in QT interval was less than 10 milliseconds.   

Secondary endpoints included the 24-hour time-weighted average increase in QT interval and categorical analyses of clinically significant individual outliers. The 24-hour time-weighted average increase in QT interval for oliceridine was 4.0 milliseconds. There were no individual outliers with a rate-corrected change from baseline greater than 60 milliseconds or an absolute QT interval greater than 500 milliseconds.

In February 2020, we resubmitted the NDA for oliceridine based on thereport topline data from the healthy volunteer QTthis study and the final minutesmid-2022.

OLINVYK Commercialization

We initiated commercial launch of the Type A meeting with the FDA. Our resubmission package included data from the healthy volunteer QT study, nonclinical data that confirmed levels of the 9662 metabolite, and drug product validation reports. The resubmission package also specified a maximum daily dose of 27 mg, as previously acknowledged by the FDAOLINVYK in the Type A meeting minutes. Infirst quarter of 2021 with a customer-facing team of approximately 40 individuals across a range of roles including Key Account Managers, Institutional Account Managers and other professionals. We have recently updated our commercial approach focusing on burn, colorectal and cardiothoracic surgery primarily occurring in the acknowledgment letter, the FDA stated thatin-patient setting. We have also adjusted our resubmission was a complete, class 2 responsecommercial footprint to the CRL. As a result, the FDA set a PDUFA goal date of August 7, 2020 for the completion of its review of the NDA.include primarily Key Account Managers and Market Access roles (i.e., Directors or National Account).

Commercialization

According to 2017 IQVIA hospital charge detail data, approximatelyApproximately 45 million hospital patients in the United States were treated with an IV opioid infor acute pain, with the hospital setting. The majority of doses in the inpatient setting. We estimate that 9 million of these patients are at increased risk of opioid-related adverse events such as respiratory depression or post-operative nausea and vomiting. Many of these patients are elderly and have comorbid conditions, driving surgical complexity and a potential for an increased length of stay. This growing patient population results in a significant cost burden to the hospital system, and we have completed health economic analyses framing significant cost savings due to OLINVYK relative to conventional IV opioids administered werein these patients. We intend to publish these data in the peer-reviewed medical literature.

We believe the greatest opportunity for OLINVYK will be in the inpatient setting where approximately 15 million patients wereare treated with multiple doses, for an average of onefrequently over multiple days. Due to two days. Patients treated in the hospital outpatient or ambulatory surgical centers may also receive one or two doses of IV opioids for postsurgical or medical pain. The Centers for Disease Control and Prevention, or CDC, has estimated that approximately 100 million surgical and invasive diagnostic procedures occur annually in the United States. Accordingly, if approved, we believe that there is a large potential commercial opportunity for oliceridine in the management of both surgical and medical acute pain in hospital and ambulatory surgical centers.

If oliceridine ultimately receives regulatory approval, we plan to commercialize it in the United States, either on our own or with a commercial partner. Outside the United States, we expect to continue to seek collaborators to commercialize oliceridine to offset risk and preserve capital.

To commercialize oliceridine in the United States, we intend to utilize a hospital-focused specialty sales force targeting surgeons, anesthesiologists, hospitalists, and other healthcare providers with acute post-surgical or medical pain management responsibility. While we believe that the greatest opportunity for oliceridine will ultimately be in the hospital inpatient setting where acute pain is typically more severe, theits quick onset and duration of analgesia, seen with oliceridine may beOLINVYK is also well suited tofor use in the growing hospital outpatient and ambulatory surgical centers. Hospital trend data also indicates that ambulatory surgical procedures now outnumber and are growing faster than inpatient surgeries in the United States.center settings. Because many surgeons and anesthesiologists manage both inpatient and outpatient cases, we believe that early physician experiences with oliceridineOLINVYK in ambulatoryoutpatient surgery may support subsequent expansion of use into the inpatient setting.

We estimate that approximately nine million IV opioid treated hospital inpatients may be at increased risk of opioid-related adverse events such as respiratory depression or post-operative nausea and vomiting. We believe that many of these patients are elderly and have comorbid conditions, driving inpatient surgical complexity and length of stay. Population and hospital trend data indicates that these patient groups will continue to grow and be an area of focus

for inpatient care. Managing these patients and adverse events results in a significant cost burden to the hospital system. Given these changing dynamics in the hospital marketplace and the increased emphasis on clinical and economic outcomes, we expect our commercialization plans to include health economic information framing the budget impact of oliceridine through a potential reduction in the adverse events seen with conventional IV opioids in these patients.

According to 2017 data from Symphony Health Solutions, approximatelyApproximately 1,200 U.S. hospitals are responsible for approximately 70% of the annual volume of conventional IV opioid drugs prescribed.prescribed, according to 2017 data from Symphony Health Solutions. We expect to identifyhave identified a subset of these high volume hospitals that utilize high volumeshave a concentration of targeted colorectal and cardiothoracic surgeries. In addition, we are prioritizing burn centers as a setting where OLINVYK may address a significant need. Every year there are approximately 30,000 burn-related hospitalizations in the United States, with an average length of stay of 8-9 days. IV opioids inare an essential component of pain management in this setting, and have rapidly adopted new brandedthere remains a need for analgesic agents inoptions that provide rapid, long-lasting acute pain relief.

We are committed to the pastethical promotion of OLINVYK. The Company’s goal is not to increase opioid usage; rather, the Company and its representative are asking healthcare professionals to consider OLINVYK as a differentiated alternative versus conventional IV opioids when an IV opioid is necessary to manage the initial account targets for oliceridine at launch. We will work to secure Pharmacy and Therapeutics Committee approval and subsequent utilization of oliceridine at these hospitals.patient’s acute pain.

Manufacturing

We have completed process development of the active pharmaceutical ingredient, or API, in OLINVYK and have manufactured multiple commercial scalecommercial-scale batches using our proposed commercial process under current good manufacturing practices, or cGMP, conditions.cGMP. We also have completed drug product process development and have manufactured multiple commercial-scale batches of drug product using the proposed commercial process under cGMP conditions.

For oliceridine,OLINVYK, we have established commercial supply agreements for the manufacture of the API and finished (compounded, filled and packaged) drug product. Sterling Pharma Solutions (formerly Alcami Corporation,Corporation), or Alcami,

Intellectual property

Our oliceridineWe wholly own the OLINVYK patent portfolio, is wholly owned by us. The portfolio includes fourincluding five issued U.S. patents (U.S. Patent Nos. 8,835,488, 9,309,234, 9,642,842,8,835,488; 9,309,234; 9,642,842; 9,849,119 and 9,849,119)11,077,098), which claim, among other things, oliceridine,OLINVYK, compositions comprising oliceridine,OLINVYK, and methods of using oliceridine.OLINVYK. The issued patents are expected to expire no earlier than 2032, subject to any disclaimers or extensions, and any U.S. patent to issue in the future is also expected to expire no earlier than 2032, subject to any disclaimers or extensions. We also have issued patents in Australia, China, Eurasia, Europe, Hong Kong, Macau, Israel, Japan, India, South Korea, and New Zealand, which claim, among other things, oliceridine,OLINVYK, compositions comprising oliceridineOLINVYK and methods of making or using oliceridine. The foreign portfolio also includes an application that has been allowed by the European Patent Office, which claim among other things, oliceridine, compositions comprising oliceridine and methods of using oliceridine.OLINVYK. We have patent applications pending in the United States, Europe, Japan, Israel, South Korea, Brazil, Canada, and India.Canada. The issued patents and patents that could issue in the future from these allowed or pending applications outside the United States are expected to expire no earlier than 2032, subject to any disclaimers or extensions. Following the FDA approval of OLINVYK, the FDA has added four issued U.S. patents to the Orange Book of Approved Drug Products with Therapeutic Equivalence Evaluations (U.S. Patent Nos. 8,835,488, 9,309,234, 9,642,842, and 11,077,098). In addition, the Company has filed Patent Term Extension applications with the United States Patent and Trademark Office that could extend the life of one

Key findings of the study included: