• Center on Health Equity and Access
  • Clinical
  • Health Care Cost
  • Health Care Delivery
  • Insurance
  • Policy
  • Technology
  • Value-Based Care

Continuity of Care and Changes in Medication Adherence Among Patients With Newly Diagnosed Diabetes

Publication
Article
The American Journal of Managed CareFebruary 2016
Volume 22
Issue 2

This study identified 4 distinct medication adherence trajectories and found that continuity of care was consistently associated with medication adherence in every trajectory group.

ABSTRACT

Objectives: Recent studies have revealed significant variation in medication adherence among patients with chronic conditions. Little is known about the effect of continuity of care (COC) on changes in medication adherence. This study aims to identify medication adherence trajectories among patients with newly diagnosed diabetes, as well as to examine the association of COC and medication adherence among various adherence trajectories.

Methods: This study utilized a longitudinal design with a 6-year follow-up, from 2002 to 2008, under a universal health insurance program in Taiwan. Subjects 18 years or older with type 2 diabetes that was newly diagnosed in 2002 were included in the study. The main outcome was medication adherence measured by medication possession ratio each year. Group-based trajectory models were used for analysis.

Results: Four medication adherence trajectories were identified: persistent adherence (39.9%), increasing adherence (27.5%), decreasing adherence (12.0%), and nonadherence (20.6%). Patients with high or medium COC index scores were more likely to be adherent to medications than those with low COC index scores in all of the trajectory adherence groups.

Conclusions: This study demonstrated the heterogeneity in patients’ medication adherence and identified 4 distinct trajectories of medication adherences among those with newly diagnosed type 2 diabetes. Improving COC may lead to better medication adherence in all of the adherence trajectory groups.

Am J Manag Care. 2016;22(2):136-142

Take-Away Points

This study employed longitudinal data to identify medication adherence trajectories among patients with newly diagnosed diabetes and to examine the relationship between continuity of care (COC) and medication adherence among various adherence trajectories.

  • This study demonstrated the heterogeneity in medication adherence and identified 4 distinct trajectories of medication adherence: persistently high, increasing, decreasing, and nonadherence.
  • Better COC between patients and their physicians was consistently associated with higher medication adherence in every trajectory adherence group.
  • More attention should be directed toward designing new strategies to improve COC.

Diabetes is a prevalent condition characterized by significant complications and serious consequences.1 Medication adherence is the most important determinant of diabetes management; its effects are greater than those of dietary control or lifestyle changes.2 However, medication adherence rates vary markedly, from 36% to 93%, among patients with diabetes.3 Nonadherence to medications is associated with worse glycemic control, which, in turn, can increase micro- or macrovascular complications and healthcare utilization.4 Therefore, improving adherence to medications is an important task for policy makers worldwide. Medication adherence is also one of the main issues considered in value-based insurance design.5

Although the issues that affect medication adherence have been examined, 2 gaps remain in our knowledge about this issue. First, the majority of studies concerning medication adherence have used a static measure of medication adherence (ie, at a single point in time).6-10 The few studies that have used a longitudinal design either did not focus on the dynamic changes in medication adherence,11-14 or only focused on the changes between 2 time points.15,16 Furthermore, studies focusing on the changes between 2 time points could not capture the heterogeneity in medication adherence changes that occur after the second time point. Until now, only 2 studies utilized advanced dynamic measurement, capturing the short-term heterogeneity in medication adherence and examining the factors affecting the trajectory patterns of medication adherence.17,18

Continuity of care (COC) is significantly associated with favorable health outcomes, especially among patients with chronic conditions.19,20 These patients usually receive care from several physicians and have complex medication regimens that often result in fragmented care. The medical home demonstration project in the United States intends to improve care coordination among various healthcare providers, and thus improve COC between patients and their physicians.21 However, the majority of previous studies have focused on the effects of COC on healthcare utilization and patient satisfaction.22 There is limited and inconclusive evidence regarding the effects of COC on medication adherence.13,14,23-25 Furthermore, to the best of our knowledge, the effects of COC on medication adherence among patients with various adherence trajectories have been relatively unexplored.

Group-based trajectory models may provide an alternative approach to modeling the change of outcomes and individual differences in changes of outcomes.26 Its purpose is to discover distinctive patterns of individuals with homogeneous longitudinal trajectories within the population and to explain individual-level differences at the group level.27,28 Using group-based trajectory analysis, this study aimed to identify medication adherence trajectories within 6 years after the initial diagnosis of diabetes, and to examine the association of COC and long-term medication adherence among patients with various adherence trajectories.

Healthcare Delivery in Taiwan

Healthcare systems in Taiwan and in many Asian and Central and Eastern European countries largely focus on specialist and hospital care. There is no referral requirement; patients are free to visit physicians at community clinics or hospital outpatient departments for each episode according to individual preference.29 Since the implementation of the compulsory National Health Insurance (NHI) program in Taiwan in 1995, empirical studies have found that the NHI has significantly improved general access to healthcare.30 The average number of annual physician visits in Taiwan is one of the highest in the world, with approximately 13 visits per person in 2010; patients are often criticized for their doctor-shopping behavior.31 Therefore, the features of having free choice of providers for every visit without referral requirement and a very high number of physician visits under the NHI program might hamper information sharing or mutual trust between patients and their physicians; this can subsequently result in the deterioration of COC and poor patient adherence to medications. The easy access to ambulatory care and comprehensive claims data under the universal health insurance system facilitates the need for investigations into the effects of COC on medication adherence among patients with diabetes.

METHODS

Data Source and Subjects

The NHI claims data set from 1999 to 2008 was obtained from the National Health Research Institutes of Taiwan. A longitudinal study design was used for this study. We identified patients with type 2 diabetes (T2D) according to the International Classification of Diseases, Ninth Revision, Clinical Modification (ICD-9-CM) codes of 250.xx, excluding the type 1 diabetes codes of 250.x1 and 250.x3, in the claims data. First, we defined the index date of the first claim with the diagnosis of T2D for each patient in the year 2002. New patients with T2D were identified by their lack of T2D-related claims over the 3 years (1999-2002) before the index date of diagnosis in 2002.

Patients were then included in the analysis if they: 1) were aged at least 18 years on the index date; 2) were alive throughout the study period to ensure comprehensive follow-up observations; 3) had at least 3 physician visits in every year of the study period given the inapplicability of COC indicators in patients with very few visits (this criterion has been adopted in previous studies32-34); 4) had a prescription for 1 or more oral antihyperglycemic medication on the index date of the initial diagnosis to capture the appropriate timing of initial prescriptions for new patients15; 5) had at least 1 prescription for an oral antihyperglycemic medication in every year of the study period to ensure that the patients included in the study were those who required ongoing pharmacological therapy; and 6) had no insulin prescriptions during any of the years in the study period. The unit of analysis was patient-years. As a result, a total of 12,123 patients and 72,738 patient-years were included in the analysis.

Variables of Interests

Continuity of care. COC was the main independent variable in this study. This study calculated the COC score based on outpatient services only. Considering the variation and very high number of physician visits in Taiwan, we chose the continuity of care index (COCI) as our predictor variable because the COCI is minimally sensitive to the number of physician visits by patients.35 The COCI was composed of the number of different physicians seen and the number of visits to each physician. The COCI value ranges between 0 and 1, with a higher value representing better COC. The equation for the COCI is available in the PDF. N represents the total number of physician visits, nj is the number of visits to the same physician (j), j is a given physician, and M is the number of physicians. In a study by Bice and Boxerman (1977),36 the summation term in the numerator was the sum of the number of unreferred physicians. Because of the lack of referral arrangements in Taiwan, we used the total number of physician visits in the analysis. Also, because the COCI values have no inherent clinical meaning, we categorized them into 3 equal tertiles (low [0-0.23], intermediate [0.24-0.43], and high [0.44-1.00]) according to the distribution of scores across the entire study population for each year.

Medication adherence trajectory. Medication adherence was defined using the medication possession ratio (MPR), which was calculated as the ratio of the total days with a supply of a prescribed medication divided by the total number of days in each year during the 6 years following the index date. The MPR calculation also included medication days based on refill visits for oral antihyperglycemic drugs.

Antihyperglycemic drugs were identified by their anatomical therapeutic chemical codes and included biguanides (A10BA), sulfonamides or urea derivatives (A10BB), combinations of oral blood glucose—lowering drugs (A10BD), alpha glucosidase inhibitors (A10BF), thiazolidinediones (A10BG), dipeptidyl peptidase 4 (DPP-4) inhibitors (A10BH), and other blood glucose-lowering drugs, excluding insulin (A10BX). When the patients were hospitalized, the days on which they took the prescribed medications were excluded from the denominator in the MPR calculation. In addition, the patients may have received multiple medications for different numbers of days during a visit; therefore, the calculation of MPR was based on the prescription that covered the longest days (usually for chronic conditions such as diabetes). In this study, patients were considered to be adherent to oral antihyperglycemic medications if the MPR was between 80% and 120% for each year.37,38 The trajectories of medication adherence were constructed using the adherence statuses in the 6 years after the initial diagnosis of diabetes.

Covariates

Several confounding factors were controlled for in the regression models. The time-varying variables were health status measures, including: 1) hospitalization in the previous year; 2) the diabetes complication severity index (DCSI)39; 3) the chronic illness with complexity index (CICI)40; and 4) multiple medications in a prescription. The DCSI was used to adjust for the severity of diabetes complications and consisted of scores from 7 categories of complications: cardiovascular complications, nephropathy, retinopathy, peripheral vascular disease, stroke, neuropathy, and metabolic disorders. The CICI was used to adjust for comorbidity in patients with multiple chronic diseases. We excluded diabetes-related complications to avoid duplicating the comorbidity effect presented by the DCSI. In the analysis, we counted the number of comorbidities based on the CICI scores. The multiple medications per prescription were dichotomized by 3 medications or more.

The time-constant variables were the patient’s sex, age, and the location of residence (rural or urban) in the baseline year. Due to a lack of information on a patient’s residence in the NHI claim data, we took 2 steps to approximate the residence for each patient. First, we identified 3 types of beneficiaries who were enrolled into NHI via occupational unions or local government agencies—farmers and fishermen/members of occupational unions, low-income families, and local residents who were enrolled via household registry office—where the zip code of enrollment organization was considered as the proxy for patient’s residence. For the abovementioned subjects, this study only included the NHI policy holders and their spouses because they were presumably living together. For the remaining subjects, we used the zip code of the most frequently visited clinic/hospital for minor illnesses (ICD-9-CM codes 460-466, 480-487) as proxies. Rural-urban designations were based on the population density of the township of the patient’s residence. Those townships with the lowest 30% of population density were defined as a rural area in Taiwan.

Statistical Analysis

We used a semi-parametric, group-based trajectory model to identify distinct subgroups of individuals who followed similar patterns of medication adherence over time.26,41 This model was performed with the SAS version 9.2 PROC TRAJ procedure (SAS Institute, Cary, North Carolina).

We employed the Bayesian information criterion (BIC) to determine the optimal number of trajectories. Because of the large sample size in this study, we anticipated that the BIC value might decrease along with the increase in the number of trajectories; nonetheless, we only considered 1 to 4 trajectories to facilitate the interpretation of the adherence patterns from a practical perspective. Then, we determined the shape of the trajectories by testing the cubic terms of time for each trajectory first, indicating the use of cubic terms of time to model the probability that a patient within each trajectory would be adherent. To ensure the principle of parsimony, if the cubic and quadratic terms were not significant in a given model, subsequent analysis was performed with constant and linear terms.42 Once the optimal number and shape of the trajectories were chosen, we estimated the group membership probability for each subject and assigned each subject to the specific trajectory group with the highest group membership probability. Because the distribution of medication adherence was binary, we fit a logit model to examine the relationship between COC and medication adherence while taking into account the time-constant and time-varying covariates.

RESULTS

Table 1

presents the characteristics of the study subjects with newly diagnosed T2D in 2002. The mean MPR value was 75.18% and the COCI score was 0.39; the mean age was 55.62 years and males comprised 52.82% of the sample. Regarding health status, the rate of hospitalization in the previous year was 17.17%; 60.66% of the subjects had a DCSI score of 0 and 15.61% had a score of 2 or higher.

eAppendix 1

eAppendix 2

Figure

Using the group-based trajectory model, we identified 4 distinct medication adherence trajectories based on the BIC scores ( and [eAppendices available at www.ajmc.com]). As shown in the , the persistent adherence trajectory accounted for 39.9% of the subjects, and their medication adherence was constantly high. The increasing adherence trajectory accounted for 27.5% of the subjects, who showed an increasing trend in their adherence status over time, whereas the decreasing adherence trajectory included 12% of the subjects who showed a continuous declining trend in their medication adherence. The nonadherence trajectory accounted for 20.6% of the subjects, and this group consistently had the lowest probability of medication adherence.

Table 2

presents the relationship between COC and the likelihood of medication adherence among various adherence trajectories. The COCI score estimate was positively and significantly associated with medication adherence in each trajectory group. This association implies that patients with high or medium COCI scores were more likely to adhere to medication use compared with patients with low COCI scores, regardless of their trajectory groups. In addition, older patients or female patients were less likely to be in the nonadherence trajectory group than in other groups. Patients living in the rural area were more likely to be in the nonadherence trajectory group than in other groups.

DISCUSSION

The objective of this study was to construct trajectories of medication adherence among patients with newly diagnosed T2D first, and then to examine the association between COC and medication adherence among the various adherence trajectories.

Previous studies that constructed medication trajectories were restricted to short-term follow-up. Riegel et al (2012) examined the trajectories of medication nonadherence in adults with heart failure over a 6-month period and identified 2 distinct trajectories,17 and Franklin et al (2013) described patients’ adherence to the lipid-lowering medication “statin” during the 15 months following the first prescription.18

The present study identified 4 distinct medication adherence trajectories (persistent, increasing, decreasing, and nonadherence) during the 6-year follow-up period after the initial diagnosis of diabetes. We noticed that only 39.9% of the subjects were always adherent to medication and that 20.6% of the subjects were consistently nonadherent during these 6 years. We also found that older patients were less likely to be in the nonadherence trajectory group. The findings were consistent with previous studies which suggested that adherence increases with age.43,44 In addition, this study revealed that patients living in the rural area were more likely to be in the nonadherence trajectory. On the contrary, Egede et al (2011) reported that adherence to antidiabetic medication was higher among rural versus urban veterans; however, when accounting for the effect of race/ethnicity on medication adherence, they identified that rural-dwelling Hispanic veterans had lower medication adherence compared with their urban counterparts.45 The factors associated with the medication adherence patterns deserve further investigation.

Among the 4 medication adherence trajectories, we found that medication adherence was positively associated with the degree of COC. The findings of this study are consistent with those of previous studies13,14,23; however, Robels and Anderson (2011) found that a positive association between COC and adherence to antihypertensive drugs may exist only within a limited range of illness severity.25 This positive association between COC and medication adherence may be attributable to better information sharing and better goal alignment between patients and physicians, as suggested by Donaldson (2001).46

Better information sharing implies that physicians are more familiar with the patients’ prognosis and medication use over time. Better alignment between goals and treatments may increase the interpersonal relationship between patients and physicians, which, in turn, increases the patients’ trust.47,48 Increased communication and trust may, subsequently, improve patients’ medication management by improving adherence to medications, for example. This finding suggests that COC is an important factor that influences medication adherence for patients with T2D, regardless of the type of medication adherence trajectory.

Strategies that aim to increase the COC between patients and physicians should be encouraged; for example, the introduction of the medical home project in the United States21 to enhance coordinated care for patients might improve the COC for project enrollees.

Limitations

This study has several limitations. First, this study did not include unobserved (eg, health-seeking behavior) or unavailable (eg, illness severity) characteristics in the regression models. We included several proxy indicators for illness severity in the regression model, such as the DCSI score, which might reduce the bias related to the confounders that were not incorporated into the models. Second, MPR only indicates medication possession rather than medication consumption, which may lead to an overestimation of medication adherence. Nevertheless, MPR has been commonly used in previous studies to quantify medication adherence and is a valid predictor of healthcare outcomes.6-10,37,38 Third, patients without medication prescription at the first time of diabetes diagnosis and patients who received insulin treatment in any of the years during the study period were excluded from the analysis, which might lessen the representativeness of the study subjects. Finally, there are certain unique aspects of Taiwan’s healthcare system, such as free choice of providers for every visit without referral requirements, which may limit the generalizability of the findings to other healthcare systems.

CONCLUSIONS

This study demonstrated the heterogeneity in medication adherence and identified 4 distinct trajectories of medication adherence for patients with newly diagnosed T2D. Better COC between patients and their physicians was consistently associated with higher medication adherence in the 4 trajectory adherence groups. More attention should be directed toward designing new strategies to improve COC after the diagnosis of diabetes.

Author Affiliations: Department of Public Health, College of Medicine, Fu Jen Catholic University (CCC), New Taipei City, Taiwan; Institute of Health Policy and Management, College of Public Health, National Taiwan University (SHC), Taipei City, Taiwan.

Source of Funding: The study was supported by the grants from the Ministry of Science and Technology (MOST 103-2410-H-002-202-MY3; MOST 104-2410-H-030-087-MY2) and the National Health Research Institute (NHRI-EX104-10225PI) in Taiwan. The funding source had no role in the study.

Author Disclosures: The authors report no relationship or financial interest with any entity that would pose a conflict of interest with the subject matter of this article.

Authorship Information: Concept and design (SHC); acquisition of data (SHC); analysis and interpretation of data (CCC; SHC); drafting of the manuscript (CCC; SHC); critical revision of the manuscript for important intellectual content (SHC); statistical analysis (CCC); provision of patients or study materials (SHC); obtaining funding (SHC); administrative, technical, or logistic support (CCC); and supervision (SHC).

Address correspondence to: Shou-Hsia Cheng, PhD; Institute of Health Policy and Management, College of Public Health, National Taiwan University, 17 Xu-Zhou Rd, Taipei, Taiwan, 100. E-mail: shcheng@ntu.edu.tw.

REFERENCES

1. Bethel MA, Sloan FA, Belsky D, Feinglos MN. Longitudinal incidence and prevalence of adverse outcomes of diabetes mellitus in elderly patients. Arch Intern Med. 2007;167(9):921-927.

2. Hearnshaw H, Lindenmeyer A. What do we mean by adherence to treatment and advice for living with diabetes? a review of the literature on definitions and measurements. Diabet Med. 2006;23(7):720-728.

3. Cramer JA. A systematic review of adherence with medications for diabetes. Diabetes Care. 2004;27(5):1218-1224.

4. Asche C, LaFleur J, Conner C. A review of diabetes treatment adherence and the association with clinical and economic outcomes. Clin Ther. 2011;33(1):74-109. doi:10.1016/j.clinthera.2011.01.019.

5. Chernew ME, Rosen AB, Fendrick AM. Value-based insurance design. Health Aff (Millwood). 2007;26(2):w195-w203.

6. Hepke KL, Martus MT, Share DA. Costs and utilization associated with pharmaceutical adherence in a diabetic population. Am J Manag Care. 2004;10(2, pt 2):144-151.

7. Lau DT, Nau DP. Oral antihyperglycemic medication nonadherence and subsequent hospitalization among individuals with type 2 diabetes. Diabetes Care. 2004;27(9):2149-2153.

8. Sokol MC, McGuigan KA, Verbrugge RR, Epstein RS. Impact of medication adherence on hospitalization risk and healthcare cost. Med Care. 2005;43(6):521-530.

9. Ho PM, Rumsfeld JS, Masoudi FA, et al. Effect of medication nonadherence on hospitalization and mortality among patients with diabetes mellitus. Arch Intern Med. 2006;166(17):1836-1841.

10. Karve S, Cleves MA, Helm M, Hudson TJ, West DS, Martin BC. An empirical basis for standardizing adherence measures derived from administrative claims data among diabetic patients. Med Care. 2008;46(11):1125-1133.

11. Balkrishnan R, Rajagopalan R, Camacho FT, Huston SA, Murray FT, Anderson RT. Predictors of medication adherence and associated health care costs in an older population with type 2 diabetes mellitus: a longitudinal cohort study. Clin Ther. 2003;25(11):2958-2971.

12. Roebuck MC, Liberman JN, Gemmill-Toyama M, Brennan TA. Medication adherence leads to lower health care use and costs despite increased drug spending. Health Aff (Millwood). 2011;30(1):91-99. doi:10.1377/hlthaff.2009.1087.

13. Chen CC, Tseng CH, Cheng SH. Continuity of care, medication adherence, and health care outcomes among patients with newly diagnosed type 2 diabetes: a longitudinal analysis. Med Care. 2013;51(3):231-237. doi:10.1097/MLR.0b013e31827da5b9.

14. Hong JS, Kang HC. Relationship between continuity of ambulatory care and medication adherence in adult patients with type 2 diabetes in Korea: a longitudinal analysis. Med Care. 2014; 52(5):446-453. doi:10.1097/MLR.0000000000000110.

15. Hong JS, Kang HC. Relationship between oral antihyperglycemic medication adherence and hospitalization, mortality, and healthcare costs in adult ambulatory care patients with type 2 diabetes in South Korea. Med Care. 2011;49(4):378-384. doi:10.1097/MLR.0b013e31820292d1.

16. Jha AK, Aubert RE, Yao J, Teagarden JR, Epstein RS. Greater adherence to diabetes drugs is linked to less hospital use and could save nearly $5 billion annually. Health Aff (Millwood). 2012;31(8):1836-1846. doi:10.1377/hlthaff.2011.1198.

17. Riegel B, Lee CS, Ratcliffe SJ, et al. Predictors of objectively measured medication nonadherence in adults with heart failure. Circ Heart Fail. 2012;5(4):430-436. doi:10.1161/CIRCHEARTFAILURE.111.965152

18. Franklin JM, Shrank WH, Pakes J, et al. Group-based trajectory models: a new approach to classifying and predicting long-term medication adherence. Med Care. 2013;51(9):789-796. doi:10.1097/MLR.0b013e3182984c1f.

19. Miller TE. Managed care regulation: in the laboratory of the states. JAMA. 1997;278(13):1102-1109.

20. Cheng SH, Chen CC. Effects of continuity of care on medication duplication among the elderly. Med Care. 2014;52(2):149-156. doi:10.1097/MLR.0000000000000042.

21. Iglehart JK. No place like home—testing a new model of care delivery. N Engl J Med. 2008;359(12):1200-1202. doi:10.1056/NEJMp0805225.

22. van Walraven C, Oake N, Jennings A, Forster AJ. The association between continuity of care and outcomes: a systematic and critical review. J Eval Clin Pract. 2010;16(5):947-956. doi:10.1111/j.1365-2753.2009.01235.x.

23. Charney E, Bynum R, Eldredge D, et al. How well do patients take oral penicillin? a collaborative study in private practice. Pediatrics. 1967;40(2):188-195.

24. Kerse N, Buetow S, Mainous AG 3rd, Young G, Coster G, Arroll B. Physician-patient relationship and medication compliance: a primary care investigation. Ann Fam Med. 2004;2(5):455-461.

25. Robles S, Anderson GF. Continuity of care and its effect on prescription drug use among Medicare beneficiaries with hypertension. Med Care. 2011;49(5):516-521. doi:10.1097/MLR.0b013e31820fb10c.

26. Jones BL, Nagin DS. Advances in group-based trajectory modeling and an SAS procedure for estimating them. Sociol Methods Res. 2007;35(4):542-571. doi:10.1177/0049124106292364.

27. Nagin DS. Analyzing development trajectories: a semiparametric group-based approach. Psychol Methods. 1999;4(2):139-157.

28. Nagin DS. Group-Based Modeling of Development. Cambridge, MA: Harvard University Press; 2005.

29. Cheng TM. Taiwan’s new National Health Insurance program: genesis and experience so far. Health Aff (Millwood). 2003;22(3):61-76.

30. Chen L, Yip W, Chang MC, et al. The effects of Taiwan’s National Health Insurance on access and health status of the elderly. Health Econ. 2007;16(3):223-242.

31. Chen TJ, Chou LF, Hwang SJ. Patterns of ambulatory care utilization in Taiwan. BMC Health Serv Res. 2006;6:54-61.

32. Gill JM, Mainous AG 3rd. The role of provider continuity in preventing hospitalizations. Arch Fam Med. 1998;7(4):352-357.

33. Gill JM, Mainous AG 3rd, Nsereko M. The effect of continuity of care on emergency department use. Arch Fam Med. 2000;9(4):333-338.

34. Brousseau DC, Meurer JR, Isenberg ML, Kuhn EM, Gorelick MH. Association between infant continuity of care and pediatric emergency department utilization. Pediatrics. 2004;113(4):738-741.

35. Smedby O, Eklund G, Eriksson EA, Smedby B. Measures of continuity of care. a register-based correlation study. Med Care. 1986;24(6):511-518.

36. Bice TW, Boxerman SB. A quantitative measure of continuity of care. Med Care. 1977;15(4):347-349.

37. Stroupe KT, Teal EY, Tu W, Weiner M, Murray MD. Association of refill adherence and health care use among adults with hypertension in an urban health care system. Pharmacotherapy. 2006;26(6):779-789.

38. Chen CC, Blank RH, Cheng SH. Medication supply, healthcare outcomes and healthcare expenses: longitudinal analyses of patients with type 2 diabetes and hypertension. Health Policy. 2014;117(3):374-381. doi:10.1016/j.healthpol.2014.04.002.

39. Young BA, Lin E, Von Korff M, et al. Diabetes complications severity index and risk of mortality, hospitalization, and healthcare utilization. Am J Manag Care. 2008;14(1):15-23.

40. Meduru P, Helmer D, Rajan M, Tseng CL, Pogach L, Sambamoorthi U. Chronic illness with complexity: implications for performance measurement of optimal glycemic control. J Gen Intern Med. 2007;22(suppl 3):408-418.

41. Jones BL, Nagin DS, Roeder K. A SAS procedure based on mixture models for estimating developmental trajectories. Sociol Methods Res. 2001;29(3):374-393. doi:10.1177/0049124101029003005.

42. Helgeson VS, Snyder P, Seltman H. Psychological and physical adjustment to breast cancer over 4 years: identifying distinct trajectories of change. Health Psychol. 2004;23(1):3-15.

43. Hertz RP, Unger AN, Lustik MB. Adherence with pharmacotherapy for type 2 diabetes: a retrospective cohort study of adults with employer-sponsored health insurance. Clin Ther. 2005;27(7):1064-1073.

44. Kalsekar ID, Madhavan SS, Amonkar MM, et al. Depression in patients with type 2 diabetes: impact on adherence to oral hypoglycemic agents. Ann Pharmacother. 2006;40(4):605-611.

45. Egede LE, Gebregziabher M, Hunt KJ, et al. Regional, geographic, and ethnic differences in medication adherence among adults with type 2 diabetes. Ann Pharmacother. 2011;45(2):169-178.

46. Donaldson MS. Continuity of care: a reconceptualization. Med Care Res Rev. 2001;58(3):255-290.

47. Kao AC, Green DC, Davis NA, Koplan JP, Cleary PD. Patients’ trust in their physicians: effects of choice, continuity, and payment method. J Gen Intern Med. 1998;13(10):681-686.

48. Mainous AG 3rd, Baker R, Love MM, Gray DP, Gill JM. Continuity of care and trust in one’s physician: evidence from primary care in the United States and the United Kingdom. Fam Med. 2001;33(1):22-27.

Related Videos
Ian Neeland, MD
Chase D. Hendrickson, MD, MPH
Steven Coca, MD, MS, Icahn School of Medicine, Mount Sinai
Matthew Crowley, MD, MHS, associate professor of medicine, Duke University School of Medicine.
Susan Spratt, MD, senior medical director, Duke Population Health Management Office, associate professor of medicine, division of Endocrinology, Metabolism, and Nutrition,
Stephen Nicholls, MD, Monash University and Victorian Heart Hospital
Amal Agarwal, DO, MBA
Dr Robert Groves
Dr Robert Groves
Related Content
© 2024 MJH Life Sciences
AJMC®
All rights reserved.