Background

Obstructive sleep apnea (OSA) is a major risk factor for perioperative adverse events. However, no screening tool for OSA has been validated in surgical patients. This study was conducted to develop and validate a concise and easy-to-use questionnaire for OSA screening in surgical patients.

Methods

After hospital ethics approval, preoperative patients aged 18 yr or older and without previously diagnosed OSA were recruited. After a factor analysis, reliability check, and pilot study; four yes/no questions were used to develop this screening tool. The four questions were respectively related to snoring, tiredness during daytime, observed apnea, and high blood pressure (STOP). For validation, the score from the STOP questionnaire was evaluated versus the apnea-hypopnea index from monitored polysomnography.

Results

The STOP questionnaire was given to 2,467 patients, 27.5% classified as being at high risk of OSA. Two hundred eleven patients underwent polysomnography, 34 for the pilot test and 177 for validation. In the validation group, the apnea-hypopnea index was 20 +/- 6. The sensitivities of the STOP questionnaire with apnea-hypopnea index greater than 5, greater than 15, and greater than 30 as cutoffs were 65.6, 74.3, and 79.5%, respectively. When incorporating body mass index, age, neck circumference, and gender into the STOP questionnaire, sensitivities were increased to 83.6, 92.9, and 100% with the same apnea-hypopnea index cutoffs.

Conclusions

The STOP questionnaire is a concise and easy-to-use screening tool for OSA. It has been developed and validated in surgical patients at preoperative clinics. Combined with body mass index, age, neck size, and gender, it had a high sensitivity, especially for patients with moderate to severe OSA.

OBSTRUCTIVE sleep apnea (OSA) is the most prevalent breathing disturbance in sleep,1affecting 2–26% of the general population depending on sex, age, and the definition of criteria.2OSA is associated with significant morbidity, including excessive daytime sleepiness, loud snoring during sleep, refractory hypertension, and impaired quality of life. Studies have also shown that OSA is associated with a high risk for traffic accidents and cardiovascular disease.3,4 

The prevalence of OSA in the surgical population is higher than in the general population and varies with different surgical populations. In particular, approximately 7 of every 10 patients undergoing bariatric surgery were found to have OSA,5presumably because of the high level of obesity in this surgical population. Of even greater concern, despite OSA being present in the majority of patients presenting for bariatric surgery,5,6most cases were not diagnosed, and careful screening was not implemented before surgery.6One of the barriers to study the prevalence of OSA in surgical patients is the difficulty with recruiting patients to undergo polysomnography before surgery. Fidan et al.  7screened 433 surgical patients; only 18 of 41 invited patients agreed to undergo polysomnographic testing, and 14 patients (3.2% of all screened patients) were diagnosed with OSA. In another study conducted by Chung et al. ,824% of 305 surgical patients were classified as being at high risk of having OSA using the Berlin questionnaire, and 13 patients were confirmed as having OSA by polysomnography, 4.2% of the total number of patients screened.

It is estimated that nearly 80% of men and 93% of women with moderate to severe sleep apnea are undiagnosed.9Undiagnosed OSA may pose a variety of problems for anesthesiologists. A number of case reports have documented an increase in the incidence of postoperative complications and deaths among patients suspected of having OSA.10Untreated OSA patients are known to have a higher incidence of difficult intubation, postoperative complications, increased intensive care unit admissions, and greater duration of hospital stay.11–13Identifying patients with OSA is the first step in preventing postoperative complications due to OSA.

In-laboratory polysomnography is the accepted standard for diagnosing OSA.14However, polysomnography is a time-consuming and costly procedure. Further, the growing awareness of sleep apnea has exacerbated the long waiting list in many sleep laboratories.15To deal with this issue, a number of screening questionnaires and clinical screening models have been developed to help identify patients with OSA.16–25However, a significant limitation to the aforementioned studies is that patients were preselected because most studies were conducted in the sleep laboratory setting.16,18,19,26Furthermore, clinical models designed for OSA screening usually require the assistance of a computer and may not be suitable for clinical practice. One of the most widely used questionnaires, the Berlin questionnaire, has not been validated as a screening instrument in surgical patients. The American Society of Anesthesiologists (ASA) checklist, a screening instrument recommended by the ASA Task Force on Perioperative Management of Patients with Obstructive Sleep Apnea, has not been validated. Besides the fact that no predictive model or questionnaire for identifying OSA has been validated in the surgical patient population, most questionnaires have numerous items with a confusing scoring system. As a result, they are not suitable for a busy clinical setting, such as preoperative clinics.

The purpose of the study was to develop and validate a concise and easy-to-use questionnaire for OSA screening in surgical patients.

Patient Population of the Study

The study was conducted in the preoperative clinics of Toronto Western Hospital and Mount Sinai Hospital, Toronto, Ontario, Canada. Ethics approval was obtained from both institutions. Patients aged 18 yr or older who had an ASA physical status of I–IV and were scheduled to undergo elective procedures in general surgery, gynecology, orthopedics, urology, plastic surgery, ophthalmology, or neurosurgery were included in the study. Patients who were unwilling or unable to give informed consent, patients previously diagnosed with OSA or any other sleep breathing disorder, or patients who were expected to have abnormal electroencephalographic findings (e.g. , brain tumor, epilepsy surgery, patients with deep brain stimulator) were excluded. All patients who visited the preoperative clinics for their scheduled surgery and met the inclusion criteria were approached by the research staff. After informed consent was obtained, patients were asked to complete a questionnaire and were invited to undergo an overnight polysomnographic study.

Development of the STOP Questionnaire

To keep the questionnaire concise and easy to use, the questions were designed in yes/no format. Based on our previous work with the Berlin questionnaire,8consensus from a group of anesthesiologists and sleep specialists, and a literature review, four questions (STOP Q1–4) related to snoring, tiredness during the daytime, stopped breathing during sleep, and hypertension were designed. They were phrased in English at a fifth-grade reading level by using the Flesch-Kincaid reading-level determination method built into Microsoft Word (Microsoft, Redmond, WA).

To examine the association of the questions with the underlying constructs that the questions were designed to reflect, these four yes/no questions were combined with items 1–10 (Berlin Q1–10) from the Berlin questionnaire to make a question list consisting of 14 questions. The question list was administered to 278 patients to answer. Of these patients, 254 answered all of the questions. Factor analysis with the SAS procedure Factor was based on the responses from these 254 patients. After a significant level of association was demonstrated, these four yes/no questions were accepted to form the STOP questionnaire (appendix 1). The four-item STOP questionnaire is a self-report, forced-choice (yes/no), paper-and-pencil scale that takes approximately 1 min to complete. It consists of the following four questions: S—“Do you s  nore loudly (louder than talking or loud enough to be heard through closed doors)?” T—“Do you often feel t  ired, fatigued, or sleepy during daytime?” O—“Has anyone o  bserved you stop breathing during your sleep?” P—“Do you have or are you being treated for high blood p  ressure?”

The STOP questionnaire was given to 592 preoperative clinic patients as a pilot study. All patients who answered the STOP questionnaire were invited to undergo an overnight, technician-supervised polysomnographic study. According to the interim analysis of the data from pilot study, the cutoff point of the STOP questionnaire had been decided and the sample size had also been adjusted.

To check the reliability of the questionnaire, 55 patients answered the STOP questionnaire twice at different time intervals of 1–27 days (median, 8 days). Because these four questions reflected four different dimensions of OSA morbidity, internal consistency checking was not applicable.

Validation of the STOP Questionnaire

After the pilot study, 1,875 patients were screened and asked to complete the STOP questionnaire. All patients, regardless of their score on the STOP questionnaire, were invited to undergo an overnight polysomnographic study. The data from patients who completed the polysomnographic study was used to validate the STOP questionnaire. The predictive parameters of the STOP questionnaire versus  the apnea–hypopnea index (AHI) obtained from polysomnography in all patients of the validation group and in subgroups with different clinical characteristics—such as body mass index (BMI), age, neck circumference, and gender—were analyzed. An alternative scoring model incorporating B  MI, a  ge, n  eck circumference, and g  ender into the STOP questionnaire, termed the STOP-Bang (appendix 2), was also presented.

Sleep Study

A one-night, in-laboratory polysomnographic study was conducted before surgery at Toronto Western Hospital Sleep Laboratory. The result of polysomnography was used to evaluate the validity of the STOP questionnaire. During the overnight polysomnographic study, every patient went to bed at his or her usual bedtime. Collection of continuous sleep architectural data was accomplished using a standard electroencephalographic montage consisting of an electroencephalogram, electro-oculogram, submental electromyogram, and electrocardiogram using surface electrodes. Ancillary channels were used to specifically record respiratory parameters, including respiratory effort by thoracoabdominal excursion, respiratory inductive plethysmography, and oronasal airflow by nasal airflow pressure. Oxygen saturation was measured with a pulse oximeter.

One certified polysomnographic technologist with 10 yr of experience scored all of the polysomnographic recordings. Her scoring was under the supervision of a sleep physician (C.M.S.). The reports had to be assessed and approved by the sleep physician (C.M.S.). The certified technologist was blinded to the results of the STOP questionnaire (i.e. , whether patients were at high or low risk of having OSA) and clinical information of the patients. Sleep stages and the AHI were scored according to standard criteria.27,28To avoid bias and inaccuracy from polysomnographic scoring, the polysomnographic recording of 10 randomly selected patients was rescored by another experienced certified polysomnographic technologist, who was blinded to the scores of other technologist. The scores from two technologists for the same patient were almost identical (r = 0.984, P < 0.0001).

The clinical diagnosis of OSA was defined as AHI greater than 5 with fragmented sleep and daytime sleepiness. According to the American Academy of Sleep Medicine practice guideline, the severity of OSA is determined by the AHI: 5–15, mild; greater than 15–30, moderate; greater than 30, severe.27After polysomnography, patients were scheduled to meet with a sleep specialist (C.M.S.) for follow-up assessment and clinical management, where necessary.

Data Analysis and Statistics

Sample Size Estimation.

The calculation of sample size was performed according to the method reported by Obuchowski.29Briefly, the two separate calculations of sample size were performed based on either estimated sensitivity, the precision (potential error) of sensitivity, expected power, a type I error, and estimated prevalence; or specificity, the precision of specificity, expected power, type I error, and prevalence. The bigger number of the two is chosen as the sample size. Based on the literature on the Berlin questionnaire30–32and the prevalence of OSA,33,34a sensitivity of 0.88, a precision of 0.09, an OSA prevalence rate of 24%, a type I error of 0.05, and a power of 0.8 were used to calculated sample size. The result was 208. The number calculated based on a specificity of 0.80 was much smaller than 208. So 208 was initially chosen as the sample size. From the pilot study data, the sensitivity was 0.72 and the prevalence was 0.7. If the other parameters were kept the same, the sample size would be 137. However, a prevalence of 0.7 is very high. It may be biased because of the small number of patients in the pilot study. If, for safety, 0.55 were taken as the prevalence, the adjusted sample size would be 170.

For factor analysis, the minimum requirement for sample size is the bigger of 100 respondents or 5 times the number of variables. In our study, we had 14 questions (variables), so we needed at least 100 complete respondents. The list of 14 questions was given to 278 patients; 254 patients who answered all of the questions were used for the factor analysis.

Data Analysis.

Data were entered into a specifically designed Microsoft Access database and checked for possible errors. SAS 9.1 for Windows (SAS Institute, Cary, NC) was used for data analysis. Categorical data were presented as frequency and percentage with 95% confidence interval (CI). The statistical significance was checked by chi-square test or Fisher exact test. Resampling with bootstrap was used to calculate the CI of the likelihood ratios. A logistic regression procedure was used to calculate the odds ratio and area under the receiver operating characteristic curve. Continuous data were presented as mean ± SD, and the Student t  test or analysis of variance was used to calculate the P  value. P < 0.05 was defined as significant. The SAS procedure Factor was used for factor analysis. The report from the principal components analysis with varimax rotations was presented. Factors with an eigenvalue greater than average were retained. Questions with factor loading of 0.3 or greater were chosen for interpretation of factors.

Patient Screening

Over a period of 16 months at Toronto Western Hospital and Mount Sinai Hospital preoperative clinics, a total of 2,974 patients were willing to complete the questionnaire. Of these, 2,721 patients (91.5%) answered all of the items on the questionnaire completely and had complete documentation of gender, age, and BMI. Only these patients were included in the analysis.

Factor analysis was based on the response of 254 patients who answered all 14 questions from the STOP and Berlin questionnaires. After the STOP questionnaire was developed, it was administered to 2,467 patients. The STOP questionnaire classified 27.5% of patients (679 of 2,467) as being at high risk of having OSA. Of all patients who were invited to undergo the overnight monitored polysomnographic testing, 416 of 2,467 patients (17%) gave consent to participate. In total, 211 patients underwent polysomnography, whereas 205 did not show up at the laboratory (fig. 1). Of 211 patients who underwent polysomnography, the first 34 patients were included in a pilot study and the following 177 patients were for the validation of the STOP questionnaire.

Age, gender, and BMI of the different patient groups are shown in table 1. The patients who gave consent but did not actually undergo polysomnographic testing were younger than the group of patients who underwent the polysomnographic study. The BMI of patients who gave consent for polysomnography was significantly greater than that of the patients who did not give consent for polysomnography, regardless of whether the patient underwent polysomnographic testing. Compared with the patients who underwent polysomnographic testing, there was a higher rate of smoking in patients who gave consent but did not show up for the polysomnographic testing (26.8% vs.  14.7%; P = 0.002).

Development of the STOP Questionnaire

Four yes/no questions related to snoring, tiredness during the daytime, observed apnea during sleep, and hypertension were combined with 10 questions from the Berlin questionnaire and administered to 278 patients; 254 patients answered all of the questions. Demographic data are shown in table 1. Factor analysis demonstrated that four underlying factors were reflected by the 14 questions. These factors accounted for more than 95% of the total eigenvalue. Based on the category of questions with a loading factor greater than 0.3, four factors were identified: snoring, tiredness during daytime, cessation of breathing during sleep, and high blood pressure. The factor loading value for each question in the corresponding category is shown in table 2. The factor loading value of two questions related to falling asleep while driving (Berlin Q8 and Q9) is very low for all four factors.

Among the five questions related to snoring, although question 1 (STOP Q1) did not have the highest factor loading value, it still demonstrated a significant association with snoring. Because we wanted to develop a simple and easy-to-use questionnaire with questions in yes/no format, we chose question 1 to reflect snoring in our questionnaire. Using a similar rationale, question 6 was incorporated to reflect daytime tiredness. Regarding the cessation of breathing during sleep and high blood pressure, two questions in each category had similar factor loading values, so questions 12 and 14 were acceptable choices to reflect breathing cessation during sleep and high blood pressure in the STOP questionnaire. The final STOP questionnaire consisted of four yes/no questions: 1, 6, 12, and 14 (appendix 1).

Pilot Study

As a pilot study, the STOP questionnaire was administered to 592 preoperative clinic patients, and all patients were invited to undergo polysomnography. Thirty-four of these patients underwent the polysomnography study. The other patients either declined to give consent or gave consent but did not show up. Of 34 patients, 24 (70.5%) had an AHI greater than 5. According to the analysis of data from these 34 patients, using answering yes to two or more questions as the cutoff for the STOP questionnaire to classify the patients as high or low risk of having OSA demonstrated the best combination of sensitivity and specificity. The sensitivity of the STOP questionnaire was 72% (CI, 54.4–89.6), the specificity was 33.3% (CI, 2.5–64.1), the positive predictive value (PPV) was 75.0% (CI, 57.7–92.3), and the negative predictive value (NPV) was 30% (CI, 6.7–65.3).

To check the test–retest agreement, 55 patients answered the STOP questionnaire twice at a time interval of 1–27 days (median: 8 days); 53 (96.4%) patients were found to have the same score upon retesting with a κ coefficient of 0.923 (CI, 0.82–1.00).

Validation of the STOP Questionnaire

Demographic Data and Sleep Study.

Table 3shows the demographic data of the patients who participated in the validation study, i.e. , they completed the questionnaires and underwent polysomnography. The patients classified by the STOP questionnaire as being at high risk of having OSA had a significantly higher frequency of hypertension and gastroesophageal reflux disease. They also had significantly higher average ASA physical status, larger BMI, larger neck circumference, and higher AHI.

Using an AHI greater than 5 as the cutoff for diagnosis of OSA, 122 patients (68.9%) were found to have OSA, 52 (29.4%) mild, 31 (17.5%) moderate, and 39 (22.0%) severe. As shown in table 4, there were clear differences between patients with an AHI of 5 or less and patients with an AHI greater than 5. There was a higher percentage of male patients with an AHI greater than 5 (57% male vs.  43% female; P < 0.01). The patients with an AHI greater than 5 were almost more than 10 yr older than patients with an AHI of 5 or less. They also had significantly higher average ASA physical status and blood pressure, greater BMI, and larger neck size.

Table 5summarizes the sleep parameters in validation patients. Compared with the patients with an AHI of 5 or less, the patients with an AHI greater than 5 demonstrated a significantly increased arousal index, significantly lower minimum arterial oxygen saturation, and significantly decreased slow wave sleep, which is consistent with the sleep features of the patients with OSA.

STOP Questionnaire Effectively Identified the Patients with OSA.

Predictive parameters for the STOP questionnaire at AHI greater than 5, greater than 15, and greater than 30 cutoff values are presented in table 6. Using AHI greater than 5 as a cutoff value to evaluate the STOP questionnaire, the sensitivity was 65.6%, the specificity was 60.0%, the PPV was 78.4%, and the NPV was 44.0%. The sensitivity and NPV were 74.3% and 76.0% at AHI greater than 15. They were 79.5% and 89.3% with AHI greater than 30 as the cutoff. This indicates that the STOP questionnaire was more sensitive in detecting the patients with moderate to severe OSA.

Further examination of the predictive parameters of the STOP questionnaire in the different patient groups demonstrates that the PPV with AHI greater than 5 as the cutoff was greatly increased in patients with a certain demographics: BMI greater than 35 kg/m2, age older than 50 yr, male gender, and neck circumference greater than 40 cm (fig. 2). The PPV of those ranked by the STOP questionnaire as being at high risk of having OSA was 84% in the patients with a BMI greater than 35 kg/m2, 86.9% in patients older than 50 yr, 87.5% in male patients, 89.7% in male patients older than 50 yr, 94.3% in patients with neck circumference greater than 40 cm, and 100% in male patients older than 50 yr and with a BMI greater than 35 kg/m2.

STOP-Bang, an Alternative Scoring Model Combining BMI, Age, Neck Circumference, and Gender with the STOP Questionnaire.

To further improve the sensitivity of the STOP questionnaire to detect most patients with OSA, especially moderate and severe OSA, we developed an alternative scoring model, the STOP-Bang (appendix 2), which incorporated BMI, age, neck circumference, and gender into the scoring model of the STOP questionnaire. As shown in table 7, sensitivity and NPV are significantly increased by using the STOP-Bang. The sensitivities at AHI cutoffs of greater than 5, greater than 15, and greater than 30 were 83.6, 92.9, and 100%, respectively; the corresponding NPVs were 60.8, 90.2, and 100%.

In this study, the STOP questionnaire was developed and validated as an OSA screening tool for surgical patients. The STOP questionnaire is a self-administered screening tool that includes four yes/no questions (appendix 1). The STOP questionnaire was found to have a moderately high sensitivity and PPV at AHI greater than 5, greater than 15, and greater than 30 as cutoffs. In patients with certain clinical characteristics, such as male gender, age older than 50 yr, BMI greater than 35 kg/m2, and neck circumference greater than 40 cm, the PPV was greatly increased. When incorporating BMI, age, neck circumference, and gender into the STOP scoring (STOP-Bang), the sensitivity and NPV significantly increased. They were both more than 90% for the patients with moderate and severe OSA.

Obstructive sleep apnea is known to diminish quality of life35and is associated with many common comorbid conditions. Studies have documented an increased incidence of coronary artery diseases, hypertension, cerebrovascular accidents, gastroesophageal reflux disease, congestive heart failure, and myocardial infarction in OSA patients.36,37It is estimated that the average life span of an untreated OSA patient is 58 yr, which is 20 yr shorter than the average life span of the general population (men, 79 yr; women, 83 yr).38OSA is also associated with an increased incidence of postoperative adverse events.11–13Undiagnosed OSA in surgical patients have a serious impact on the postoperative outcome. Identifying patients with a high risk of OSA is the first step for the prevention of adverse health events, adverse perioperative outcomes, and its treatment. Screening tools work as a filter to separate the patients with a high risk of OSA from the patients with a low risk of OSA. A good screening tool should be validated in the target population against an accepted standard. It should be easy to use and have a high sensitivity and acceptable specificity.

Most screening tools for OSA so far have been validated in patients referred to sleep clinics or sleep laboratories. Seven predictive models, based on the different combinations of witnessed apneas, snoring, gasping, BMI, age, gender, and hypertension were developed and validated in the patients from sleep centers.16,18,19,21,23,24,39,40The Sleep Disorders Questionnaire,41Apnea Score,25and Global Sleep Assessment Questionnaire were all tested in patients mainly from sleep centers.42Patients referred to sleep centers are suspected of having sleep-related disorders, especially OSA. They are preselected patients. Screening tools for OSA developed and validated in the sleep center patient population cannot be applied to other patient populations without validation in the target patient population.

The Berlin questionnaire is one of the few questionnaires that have been validated in primary care patients.30However, instead of monitored polysomnography in a sleep laboratory, home portable sleep monitoring was used for the validation of the Berlin questionnaire. Home portable sleep monitoring has not been accepted as the standard for the diagnosis of OSA. The STOP questionnaire is currently the only questionnaire developed and validated in surgical patients. Although there was some self-selection from the patients' perspective, our study was designed to include all surgical patients in our preoperative clinics regardless of their score of the STOP questionnaire to avoid selection biases.

In most previous studies, reports from monitored polysomnography were used to validate models or questionnaires. However, the staff performing the polysomnography and scoring the polysomnography were usually not blinded to the score on the questionnaire.18,19,23–25,39,40,42This may have introduced bias into the scoring of polysomnography. In our study, in-laboratory polysomnography was used to evaluate the accuracy of the STOP questionnaire. The staff performing and scoring the polysomnography was blinded to the score on the STOP questionnaire. This practice avoided bias during polysomnographic scoring.

Ease of use is also very important for a screening tool in busy clinical settings. Prediction models need calculation and computer assistance. Most widely used questionnaires have a long question list with a complicated scoring system. Although the questions are similar, the number of questions among the different OSA screening tools varies. For example, there are 11 multiple-choice questions organized into three categories on the Berlin questionnaire,30and 14 items under three categories on the OSA checklist, which is recommended by the ASA.43Study has shown that the response rate among patients decreases with increasing length of the questionnaire.44Four questions on the STOP questionnaire were designed in yes/no format, and it takes less than 1 min to finish. As a result, it had a high completion rate (91.5%) and test–retest agreement (96.4%). The STOP questionnaire is based on questions referring to s  noring, t  iredness/sleepiness, o  bserved stop of breathing during sleep, and blood p  ressure. The alternative scoring model, the STOP-Bang, is based on eight items including four questions in STOP questionnaire, B  MI, a  ge, n  eck circumference, and g  ender. This creates the easy mnemonics STOP and STOP-Bang, which may serve as useful reminders for clinicians to use these instruments during the preoperative screening process.

To screen patients for a disease with an important health impact, a high sensitivity with an acceptable specificity is a basic requirement for a screening tool. The sensitivity and specificity of OSA screening tools have demonstrated considerable variability depending on the screening tool, the patient population, and the definition of OSA. For the prediction models tested in sleep center patients, the sensitivity varied from 76% to 96%, and the specificity ranged from 13% to 54%.18,19,40For the questionnaire tested in sleep center patients, the sensitivity varied from 70% to 93%.25,41,42The Berlin questionnaire is the most widely tested screening tool for OSA. The predictive parameters of the Berlin questionnaire largely varied in different patient populations. The sensitivity was 86% in primary care patients,3062.5% in patients undergoing pulmonary rehabilitation, and 57–68% in sleep laboratory patients.45The wide variation in the sensitivity of the Berlin questionnaire also indicates the risk of transferring a screening tool between different patient populations without validation in the target patient population.

In terms of the predictive parameters, the STOP questionnaire itself demonstrated a moderately high level of sensitivity and specificity in surgical patients, and it was more sensitive to detect the patients with moderate to severe OSA. In the patients with certain clinical characteristics, such as male gender, age older than 50 yr, BMI greater than 35 kg/m2, and neck circumference greater than 40 cm, the high risk of OSA ranked by the STOP questionnaire could have a very high PPV for OSA (fig. 2). On the other hand, when incorporating BMI, age, neck circumference, and gender (Bang) into the STOP model (STOP-Bang); we could reach a very high level of sensitivity and NPV, especially for the moderate and severe OSA patients (table 6). Therefore, if a patient is ranked as low risk of OSA by the STOP-Bang scoring model, we would have a high confidence to exclude the possibility that the patient would have moderate to severe OSA.

This study has several limitations. In our study, the refusal rate for polysomnography was high. Self-selection from patients may exist because patients who had sleep symptoms might have selectively consented to the overnight polysomnography. The high refusal rate and dropout rate (49% of patients did not show up for their scheduled polysomnographic testing) also indicate the difficulty that the study faced. This may be due to the anxiety about surgery and the need to stay one night in the sleep laboratory. Other factors also played a role in patient refusal and dropout, e.g. , smokers and younger patients tended not to show up for their scheduled overnight polysomnography. The high prevalence of OSA in the group of patients who underwent polysomnography may reflect this self-selection. Currently, this tool has only been tested in surgical (noncancer) patients. It needs to be validated in the other settings.

In conclusion, the STOP questionnaire is a concise and easy-to-use screening tool to identify patients with a high risk of OSA. It has been validated in surgical patients at preoperative clinics as a screening tool. The STOP-Bang scoring model, which incorporates BMI, age, neck size, and gender with the STOP questionnaire, has demonstrated a higher sensitivity and NPV, especially for patients with moderate to severe OSA.

The authors thank all of the anesthesiologists at Toronto Western Hospital, Toronto General Hospital, and Mount Sinai Hospital (Toronto, Ontario, Canada).

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Appendix 1: STOP Questionnaire

Height _____ inches/cm Weight _____ lb/kg

Age _____ Male/Female BMI _____

Collar size of shirt: S, M, L, XL, or _____ inches/cm

Neck circumference* _____ cm

  1. S  noring

    Do you s  nore loudly (louder than talking or loud enough to be heard through closed doors)?

    Yes No

  2. T  ired

    Do you often feel t  ired, fatigued, or sleepy during daytime?

    Yes No

  3. O  bserved

    Has anyone o  bserved you stop breathing during your sleep?

    Yes No

  4. Blood p  ressure

    Do you have or are you being treated for high blood p  ressure?

    Yes No

* Neck circumference is measured by staff.

High risk of OSA:  answering yes to two or more questions

Low risk of OSA:  answering yes to less than two questions

Appendix 2: STOP-Bang Scoring Model

  1. S  noring

    Do you s  nore loudly (louder than talking or loud enough to be heard through closed doors)?

    Yes No

  2. T  ired

    Do you often feel t  ired, fatigued, or sleepy during daytime?

    Yes No

  3. O  bserved

    Has anyone o  bserved you stop breathing during your sleep?

    Yes No

  4. Blood p  ressure

    Do you have or are you being treated for high blood p  ressure?

    Yes No

  5. B  MI

    B  MI more than 35 kg/m2?

    Yes No

  6. A  ge

    A  ge over 50 yr old?

    Yes No

  7. N  eck circumference

    N  eck circumference greater than 40 cm?

    Yes No

  8. G  ender

    G  ender male?

    Yes No

High risk of OSA:  answering yes to three or more items

Low risk of OSA:  answering yes to less than three items