| Literature DB >> 25906025 |
Hilde D Luijks1, Wim J C de Grauw1, Jacobus H J Bor1, Chris van Weel2, Antoine L M Lagro-Janssen1, Marion C J Biermans1, Tjard R Schermer1.
Abstract
BACKGROUND: Little is known about the association between COPD and diabetes control parameters. AIMS: To explore the association between comorbid COPD and longitudinal glycaemic control (HbA1C) and systolic blood pressure (SBP) in a primary care cohort of diabetes patients.Entities:
Mesh:
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Year: 2015 PMID: 25906025 PMCID: PMC4532160 DOI: 10.1038/npjpcrm.2015.32
Source DB: PubMed Journal: NPJ Prim Care Respir Med ISSN: 2055-1010 Impact factor: 2.871
Figure 11Patients with the GP responsible for diabetes treatment. 2A patient’s first outcome measurements collected from a diabetes check-up visit within the first 4 months since the diabetes diagnosis was labelled as ‘baseline measurement’. CMR, Continuous Morbidity Registration; COPD, chronic obstructive pulmonary disease; GP, general practitioner; SBP, systolic blood pressure.
Baseline characteristics of patient population, according to the presence/absence of COPD
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| Sex: male, | 294 (48.2) | 34 (54.0) | 260 (47.5) | 0.33 |
| Age at DM diagnosis, years; mean (s.d.) | 63.0 (12.5) | 69.0 (11.0) | 62.3 (12.5) | <0.001 |
| Follow-up time, years; mean (s.d., range) | 6.2 (4.6; 0.1–21.9) | 4.1 (3.6; 0.3–15.6) | 6.5 (4.7; 0.1–21.9) | <0.001 |
| Measurements per patient, total number, mean (median; s.d.; range) | 21.8 (17.5; 18.2; 1–106) | 15.7 (10; 14.9; 1–86) | 22.5 (19; 18.4; 1–106) | 0.001 |
| BMI at baseline | 29.8 (5.1) | 29.5 (5.2) | 29.8 (5.1) | 0.57 |
| SES | ||||
| Low | 315 (52.1) | 37 (58.7) | 278 (51.3) | 0.26 |
| Middle | 242 (40.0) | 24 (38.1) | 218 (40.2) | |
| High | 48 (7.9) | 2 (3.2) | 46 (8.5) | |
| Year of diabetes diagnosis, | ||||
| 1985–1989 | 83 (13.6) | 3 (4.8) | 80 (14.6) | 0.07 |
| 1990–1999 | 235 (38.5) | 24 (38.1) | 211 (38.6) | |
| 2000–2006 | 292 (47.9) | 36 (57.1) | 256 (46.8) | |
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| Comorbid diseases | 2.7 (2.3; 0–11) | 4.0 (2.5; 0–11) | 2.6 (2.2; 0–11) | <0.001 |
| Comorbid diseases | ||||
| 0 | 100 (16.4) | 4 (6.3) | 96 (17.6) | 0.002 |
| 1 or 2 | 227 (37.2) | 17 (27.0) | 210 (38.4) | |
| 3 and more | 283 (46.4) | 42 (66.7) | 241 (44.1) | |
| Cardiovascular comorbidity | 390 (63.9) | 44 (69.8) | 346 (63.3) | 0.30 |
| Musculoskeletal comorbidity | 197 (32.3) | 32 (50.8) | 165 (30.2) | 0.001 |
| Mental comorbidity | 140 (23.0) | 18 (28.6) | 122 (22.3) | 0.26 |
| Comorbid malignancy | 42 (6.9) | 4 (6.3) | 38 (6.9) | 0.86 |
| Incident comorbid COPD after DM diagnosis | 12 (2.0) | NA | 12 (2.2) | NA |
| Incident COPD in the first year after DM diagnosis, | 1 (0.2) | NA | 1 (0.2) | NA |
| Incident COPD in the first 5 years after DM diagnosis, | 8 (1.3) | NA | 8 (1.5) | NA |
Characteristics of patients at baseline, i.e., at the date of the diabetes diagnosis.
Abbreviations: BMI, body mass index; DM, type 2 diabetes mellitus; NA, not applicable; SES, socio-economic status.
COPD presence/absence: assessed on the date of diabetes diagnosis. P-values displayed are calculated for the difference between the group with versus without comorbid COPD. We performed Chi-square tests for continuous variables and independent t-tests for continuous variables. P-values <0.05 were considered statistically significant.
Number of measurements available for BMI at baseline: 576 (missing at baseline: n=34). Number of measurements available for SES at baseline: 605 (missing at baseline: n=5).
Presence of any type of comorbid disease was assessed at the date of diabetes diagnosis. For the diabetes patients with comorbid COPD present at the diabetes diagnosis date, we excluded COPD in the count of the total number of comorbid diseases to make a meaningful comparison with the total number of comorbid diseases in patients without COPD.
Mean time (after the diabetes diagnosis date) until the date of comorbid COPD diagnosis, for incident cases, is 4.6 years.
Figure 2Mixed model results (no subgroup effect analysis): longitudinal HbA1C (a) and SBP (b) outcomes of diabetes patients with and without comorbid COPD. Comorbid diseases: absence and presence are assessed on the date of diabetes diagnosis. Number (n) of cases with completed longitudinal analysis (no missing data on any of the variables included in the mixed model throughout): 582. Cases with missing values for BMI: n=23, cases with missing values for SES: n=5. *P-values <0.05. Age and BMI categories: based on the distribution of age and BMI values of patients contributing to the analyses, limits for ‘low’, ‘intermediate’ and ‘high’ values were 54, 64 and 72 years for age, and 26.0, 28.5 and 31.8 kg/m2 for BMI, respectively. Graphs for ‘reference categories’: in the graphic presentation, graph lines represent HbA1C or SBP courses for specific patient variables—for example, a male patient from the low-SES group with a specific age and BMI. We define the (theoretical) combination of the patient characteristics ‘male sex, low SES, median age, median BMI and absence of other comorbidity’ as ‘reference category’. The ‘Additional effects table’ below each graph contains information needed to construct lines of predicted outcomes, based on the mixed model results, for other subjects than the ‘reference category’. It shows the additional effects (to be added to the graphs displayed above) for other covariates included in the model. These values are not time dependent and not dependent on the absence or presence of COPD. Example: HbA1C courses over time for patients with and without comorbid COPD are shown in a. The ‘Additional effects table’ shows an additional effect of +0.04 (% HbA1C) for female sex. This means 0.04 should be added to the blue line for female patients without COPD and 0.04 should be added to the red line for female patients with COPD. The P-value of 0.70 shows that this additional effect of sex on HbA1C in this analysis is not statistically significant. BMI, body mass index; COPD, chronic obstructive pulmonary disease; SBP, systolic blood pressure; SES, socio-economic status.
Figure 3Mixed model results for subgroup effect analysis: 5-year course of SBP for diabetes patients with and without comorbid COPD, modified by SES (P<0.01) and BMI (P=0.03). The explanations are the same as Figure 2. Graphs are shown for the ‘reference category’ (i.e., male sex, median age, absence of other comorbidity), but SES and BMI vary as specified in the figure. BMI, body mass index; COPD, chronic obstructive pulmonary disease; SBP, systolic blood pressure; SES, socio-economic status.