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Article

Association of Anemia with Clinical Symptoms Commonly Attributed to Anemia—Analysis of Two Population-Based Cohorts

1
Faculty of Applied Health Sciences, European University of Applied Sciences, 18057 Rostock, Germany
2
Department of General Practice, Institute for Community Medicine, University Medicine Greifswald, 17475 Greifswald, Germany
*
Author to whom correspondence should be addressed.
These authors contributed equally to this work.
J. Clin. Med. 2023, 12(3), 921; https://doi.org/10.3390/jcm12030921
Submission received: 3 November 2022 / Revised: 16 January 2023 / Accepted: 20 January 2023 / Published: 24 January 2023
(This article belongs to the Section Epidemiology & Public Health)

Abstract

:
Background: Fatigue, dyspnea, and lack of energy and concentration are commonly interpreted as indicative of symptomatic anemia and may thus play a role in diagnostic and therapeutic decisions. Objective: To investigate the association between symptoms commonly attributed to anemia and the actual presence of anemia. Methods: Data from two independent cohorts of the Study of Health in Pomerania (SHIP) were analyzed. Interview data, laboratory data, and physical examination were individually linked with claims data from the Association of Statutory Health Insurance Physicians. A complete case analysis using logistic regression models was performed to evaluate the association of anemia with symptoms commonly attributed to anemia. The models were adjusted for confounders such as depression, medication, insomnia, and other medical conditions. Results: A total of 5979 participants (53% female, median age 55) were included in the analysis. Of those, 30% reported fatigue, 16% reported lack of energy, 16% reported lack of concentration, and 29% reported dyspnea and/or weakness. Anemia was prevalent in about 6% (379). The symptoms were more prevalent in participants with anemia. However, participants with anemia were older and had a poorer health status. There was no association in multivariate logistic regression models between the symptoms fatigue, lack of concentration, dyspnea, and/or weakness and anemia. Anemia was associated (OR: 1.45; 95% CI: 1.13–1.86) with lack of energy in the multivariate analysis. Other factors such as depression, insomnia, and medication were more strongly associated with the symptoms. Conclusion: The clinical symptoms commonly attributed to anemia are unspecific and highly prevalent both in non-anemic and anemic persons. Even in the presence of anemia, other diagnoses should be considered as causes such as depression, heart failure, asthma, and COPD, which are more closely associated with the symptoms. Further diagnostic research is warranted to explore the association of symptoms in different subgroups and settings in order to help clinical decision making.

1. Introduction

Anemia is a global public health problem [1] and is associated with morbidity, frailty, and mortality, including maternal and perinatal mortality [1,2,3]. The presence of anemia is an important health indicator, and its detection and treatment can potentially improve overall health [2]. Anemia has been associated with reduced quality of life, especially in people over the age of 60, which is postulated to be due to secondary effects like fatigue and a general reduction of functioning [4,5]. The causality of these associations is still debated and may be partly explained by the association of anemia with multimorbidity and inflammatory conditions [4]. Anemia is often diagnosed in routine laboratory testing as an incidental finding [6,7,8]. Symptoms of anemia described in the literature are fatigue, reduced cognitive function, dyspnea, lack of energy, weakness, and dizziness [1,5,9]. These symptoms can be interpreted as indicative of symptomatic anemia and may thus play a role in diagnostic and therapeutic decisions [10,11,12]. However, little research has been conducted on the association of the symptoms and the presence of anemia, especially when correcting for other possible causal factors.
The aim of this study was to assess the association of anemia with clinical symptoms commonly attributed to anemia in order to provide a broader base of evidence for clinicians when deciding on diagnostic work-up and on prioritizing treatment.

2. Materials and Methods

2.1. Design and Sample

This is a cross-sectional analysis using data from a prospective longitudinal cohort study in northern Germany (Study of Health in Pomerania) [13]. Data from two independent population-based SHIP cohorts (SHIP and SHIP-TREND) including data on demography, standardized laboratory measurements, and self-reported data from a computer-assisted interview were analyzed. The SHIP cohorts have been described in more detail elsewhere [13,14]. Ambulatory billing data (ICD-10 diagnoses (German modification of the 10th revision of the International Classification of Diseases)) from the Association of Statutory Health Insurance Physicians Mecklenburg-Vorpommern were individually linked with SHIP data. All participants from the second follow-up of the SHIP cohort (SHIP-2, investigation period 2008–2012; N = 2333, response to baseline 54%) and the SHIP-TREND cohort (investigation period 2008–2012, N = 4420) were eligible for inclusion [14]. Participants without billing data or informed consent for the use of billing data, with missing interview data or missing hemoglobin measurements and participants with the diagnosis chronic fatigue syndrome (ICD-Code G93.3) within 5 years prior to the SHIP-2/SHIP-TREND examination excluded from analysis (Figure 1).

2.2. Outcomes, Predictors, and Statistical Analysis

The dropout of participants between baseline and the second follow-up was considered by using inverse probability weighting (ipw). To calculate ipw, a logistic regression was performed with study participation as outcome and drop-out predicting variables from baseline investigation (age, sex, diabetes, heart failure, and stroke). The participation probability for follow-up examinations was assigned to each subject, and the reciprocal of this probability was considered in the analysis.
The outcomes fatigue, lack of energy, lack of concentration, dyspnea, and/or weakness were self-reported data from a self-assessment questionnaire. The answer categories none, mild, moderate, and severe were given for the outcomes fatigue, lack of energy, and lack of concentration. We dichotomized these variables into ‘not present’ (none and mild) and ‘present’ (moderate and severe). The answer categories for dyspnea and/or weakness were ‘only dyspnea’, ‘only weakness’, ‘both’, or ‘neither dyspnea nor weakness’. Anemia and anemia severity were defined according to the hemoglobin levels introduced by the World Health Organization (WHO). Thus, a hemoglobin level <120 g/L in women, <130 g/L in men, and <110 g/L in pregnant women was defined as anemia [15]. Iron deficiency was defined as serum ferritin <8 µg/L for women and <26 µg/L for men. Pregnancy was defined as beta-HCG ≥ 5 IU/L.
The variables extracted from billing data are defined in Table 1. Hypertension was defined as >140/90 mmHg of the average of the second and third blood pressure measurement at SHIP examination. Participants who reported moderate to severe depression, low mood, or anxiety were considered as having depression or low mood and/or anxiety. Insomnia was defined as having difficulties falling asleep more than 3 times a week (SHIP-Trend) or often (SHIP-2) or difficulties sleeping through the night (interview data). Information on medical history was obtained using the computer-assisted interview. Medications with fatigue as a side effect were identified according to the fatigue guideline by the German Society for General Practice and Family Medicine (DEGAM) [16] and included cytotoxic agents, benzodiazepines, antidepressants, antipsychotics, antihistamines, antihypertensive medications, opioids, and anti-Parkinson medications (Table 2). The Charlson Comorbidity Index (CCI) was calculated on the basis of billing diagnoses, either acute or permanent, within 1 year prior to enrollment in SHIP-2/SHIP-Trend [17].
Continuous hemoglobin levels (g/L) according to the presence of symptoms were depicted using box plots. Univariate, bivariate, and multivariate logistic regression models were applied to assess the association between anemia and the outcomes fatigue, lack of energy, lack of concentration, dyspnea, and/or weakness. We used stepwise selection to select the most suitable variables in the models. Multicollinearities among predictor variables in the same model were tested, with all correlations being <0.6. The variables ‘number of medications’ and ‘medication with fatigue as a side-effect’ could not be included in the same model because they were correlated. A sensitivity analysis was performed to determine the association of iron deficiency with anemia symptoms. We included the analysis in Supplementary Table S1. To assess if the composite of anemia symptoms was predictive of anemia, positive predictive values (PPV) of the presence of one or more anemia symptoms for the presence of anemia were calculated. The analyses were performed using SAS Institute Inc., Cary, NC, USA, Software 9.4.

3. Results

3.1. Characteristics of Study Population

A total of 5979 participants (53% female, median age 55 years) were included in the analysis. Fatigue was reported by 30%, lack of energy and lack of concentration were reported by 16% respectively, and dyspnea and/or weakness by 29% of participants (Table 3). The number of participants suffering from depression and anxiety was higher in self-reported (21%) as opposed to claims data (12%). Insomnia was reported by 24%.

3.2. Anemia

Anemia was observed in 379 (6.4%) of participants according to SHIP data. Of those, 48% were female, and the median age was 64 years. Most participants had mild anemia (78% female and 92% male) (Table 4). In participants with anemia, fatigue was reported by 34% (128/379), lack of energy by 21% (81/379), lack of concentration by 19% (70/379), and dyspnea and/or weakness by 38% (145/379). This subgroup was older and in a poorer health condition. A total of 25% had diabetes, 12% had chronic kidney disease, 7% had heart failure, and 7% had chronic obstructive pulmonary disease (Table 3). The CCI was higher among participants with anemia, as well as the number of prescribed medications and the number of medications with fatigue as a side effect. According to claims data, anemia was documented in 2.4% (43/5979) of the study population.

3.3. Association of Anemia and Symptoms

3.3.1. Fatigue

Of those who reported fatigue (30%), 7% (128/1775) had anemia. The univariate logistics regression model of anemia and fatigue revealed a weak association, which did not reach significance (OR = 1.19 (95% CI: 0.99–1.44)). The median hemoglobin levels of participants with fatigue were slightly lower than the hemoglobin levels of participants without fatigue. Overall, there was no difference in hemoglobin level distribution between participants with and without fatigue (Figure 2). In the bivariate analysis, fatigue was significantly associated with anemia after adjusting for age, sex, depression, and/or anxiety (Table S1). In the multivariate analysis, there was no association between anemia and fatigue (Table 5). Furthermore, fatigue was not associated with iron deficiency (Table S2).

3.3.2. Lack of Energy

Of those who reported lack of energy (16%), 8% (81/968) had anemia. In the univariate model, anemia and lack of energy were associated with an OR = 1.38 (95% CI: 1.11–1.70). The distribution of hemoglobin levels between participants with lack of energy compared to participants without this symptom was similar (Figure 2). In the bivariate analysis, lack of energy was significantly associated with anemia after adjusting for age, sex, hypothyroidism, depression and/or anxiety, insomnia, CCI, cancer, heart failure, diabetes, and pregnancy (Table S1). After adjusting in the multivariate model, the odds ratios for the association of anemia and lack of energy were 1.41 (95% CI: 1.09; 1.81) and 1.45 (95% CI: 1.13; 1.86), respectively (Table 5). No association was observed between lack of energy and iron deficiency (Table S2).

3.3.3. Lack of Concentration

Of those who reported lack of concentration (16%), 8% (70/927) had anemia. In the univariate analysis, anemia and lack of concentration were associated with an OR = 1.29 (95% CI: 1.03–1.61). Participants with the symptom lack of concentration had slightly lower median hemoglobin levels compared to participants without lack of concentration. Overall, the distribution of hemoglobin levels did not differ between the groups of participants with and without lack of concentration (Figure 2). In the bivariate analysis, anemia was associated with lack of concentration after adjusting for sex, hypothyroidism, depression and/or anxiety, cancer, and pregnancy (Table S1). In multivariate analysis, no significant association between anemia and lack of concentration was found (Table 5), but iron deficiency was significantly associated with lack of concentration with an OR of 1.65 (95%CI 1.24–2.19) (Table S2).

3.3.4. Dyspnea

Of those reporting dyspnea and/or weakness (30%), 8% (145/1727) had anemia. In the univariate analysis, anemia was associated with dyspnea and/or weakness with an OR = 1.55 (95% CI: 1.29–1.85). Participants with these symptoms had slightly lower median hemoglobin levels than participants without the symptoms. Overall, no difference in the distribution was observed (Figure 2). In the bivariate analysis, the association remained significant (Table S1). In the multivariate analysis, no association between anemia and dyspnea and/or weakness was observed (Table 5), and no association was observed between iron deficiency and dyspnea and/or weakness (Table S2).

3.4. Positive Predictive Value of Symptoms for the Presence of Anemia

In participants with anemia, 6.6% had all four symptoms compared to 4.7% of participants without anemia (Table 6). The positive predictive value was 8% for all four symptoms and 6% for the presence of one symptom.

3.5. Association of Symptoms with Other Variables

In the bivariate analysis, the predictors female, medication with fatigue as a side-effect, depression/anxiety, and insomnia were strongly associated with the outcomes fatigue, lack of energy, and lack of concentration (Figure 3, Figure 4 and Figure 5). The predictors heart failure, COPD, asthma, chronic kidney disease, medication with fatigue as a side-effect, and depression were strongly associated with the outcome dyspnea and/or weakness (Figure 6).
In the multivariate analysis, the predictor depression/anxiety had the strongest association with all anemia symptoms, especially with lack of energy. Number of medications, medication with fatigue as a side effect, insomnia, and an increased CCI were associated with all anemia symptoms. Heart failure, asthma, and COPD were strongly associated with dyspnea and/or weakness (Table 5).

4. Discussion

4.1. Summary of the Main Results

The prevalence of anemia in the study population was 6%. The majority of anemic subjects were classified as having mild anemia (78–92%).
Participants with anemia were older and had a higher prevalence of chronic conditions such as diabetes and chronic kidney disease, as well as a higher CCI than participants without anemia. The number of medications was higher in participants with anemia, and they used more medications with fatigue as a possible side effect. Anemia was associated with lack of energy in the multivariate logistic regression. No association was found between fatigue, lack of concentration, dyspnea, and/or weakness with anemia after adjusting for confounders, but lack of concentration was weakly associated with iron deficiency. The strongest association with anemia symptoms was found for depression and/or anxiety with an odds ratio ranging from 2.68 to 8.22. Furthermore, the symptoms were associated with polypharmacy, medications with fatigue as a possible side effect, insomnia, and CCI. Heart failure, COPD, and asthma were associated with dyspnea and/or weakness. The positive predictive value of four anemia symptoms for the presence of anemia was 8%.

4.2. Comparison with Scientific Literature

Our findings on predictivity of anemia symptoms are congruent with research by Wood (1966), who found no association between symptoms that are attributed to anemia and the presence of anemia in a survey among community dwelling adults in Great Britain [18]. In a meta-analysis of the etiology of tiredness as a symptom in general practice, the prevalence of anemia ranged from 0 to 6.9% [19]. This is in accordance with our findings, where 7% of study participants complained about fatigue and had anemia. Furthermore, they found the most common diagnosis of patients presenting with tiredness in primary care was depression, with 18.5% (95% CI: 16.2–21.0%) being diagnosed as such [19]. This is in accordance with our findings, where the strongest association of anemia symptoms was found for depression and/or anxiety. In a Dutch study among patients presenting with tiredness in general practice, Knottnerus (1986) reported no significant difference among patients and controls regarding anemia prevalence [20]. In contrast, Macher et al. (2020) reported a significant reduction in symptoms of fatigue after iron supplementation in a study among iron-deficient blood donors, but this study was neither blinded nor did it contain a control group of subjects without iron deficiency, or a placebo group [21]. Some research suggests that iron deficiency rather than hemoglobin levels may be the causal factor in some of the anemia symptoms, and that these symptoms may be alleviated by iron supplementation [22,23,24]. We found iron deficiency as indicated by low ferritin levels to be correlated with lack of concentration, but not with other anemia symptoms, in the multivariate analysis.
It is possible that the positive predictive value of anemia symptoms is higher in populations with a high a priori risk of anemia, e.g., cancer patients, who typically have high rates of anemia, ranging from 30 to 90% [25]. This is confirmed by Johnstone et al. (2020), who found a PPV of 80% for tiredness and dyspnea in a study among cancer patients, albeit with a low sensitivity of 8% [25]. Robalo Nunes et al. (2020) reported a 20% higher probability of anemia in persons with symptoms, but they recruited subjects in healthcare settings and had an extraordinarily high rate of anemia of up to 52%, which is not representative of the general population as reported by other sources, and the purported symptoms included bleeding and visible blood loss, which are causal risk factors, rather than symptoms [26].
Anemia was more prevalent in participants over the age of 50 and in participants with chronic diseases such as CKD and diabetes, leading to an increased number of medications and therefore an increased number of medications with the possible side effect of fatigue. General screening for anemia is not recommended but is usually part of CKD monitoring or prenatal care and is frequently part of standard laboratory testing [6,7]. Clinicians should consider elderly, fragile individuals and individuals with chronic diseases as a higher risk subgroup when testing for anemia.

4.3. Limitations

We conducted a complete case analysis. Due to the large sample size and the low number of excluded subjects, we do not expect a relevant influence on our results. When interpreting the results, it should be considered that most study participants had mild anemia. The low number of subjects with severe anemia did not allow further analysis of this subgroup. Additionally, SHIP cohort subjects are almost exclusively Caucasian, and thus certain genetic forms of anemia, such as hemoglobinopathy, are underrepresented. Due to the study setting, the conclusions cannot be extrapolated to in-patient clinical settings where the a priori risk of anemia is considerably higher. It is likely that the positive predictive value of anemia symptoms can be different in an in-patient population. Some research suggests that iron deficiency rather than hemoglobin levels may be the causal factor in some of the anemia symptoms and that these symptoms may be alleviated by iron supplementation [21,22,24]. In this study, we were limited to the analysis of laboratory values that were available in the SHIP-study, which included ferritin as an indicator of iron storage, but did not include hepcidin or transferrin saturation as additional indicators of iron metabolism.

4.4. Interpretation

Patients with chronic anemia often show surprisingly little symptoms, and anemia is often discovered coincidentally due to routine diagnostic testing. Although anemia has been associated with lower quality of life and several unfavorable health outcomes, this does not necessarily prove a causal relation, because of confounding factors [4].
Physicians in primary and ambulatory care often rely predominantly on patient history and symptoms when deciding on differential diagnosis and diagnostic testing. This analysis has shown that the diagnostic value of anemia symptoms is very low in the general population, which is probably inherent to the unspecific nature of the symptoms and the low prevalence of severe anemia in this population. Our data show that diagnostic work-up in patients with symptoms such as fatigue or dyspnea should not be limited primarily to anemia but rather focus on conditions such as depression, heart failure, asthma, and COPD. Because of the relatively high incidence of anemia in persons over the age of 60, age can be a useful indicator when deciding on diagnostic testing. Additionally, there is a rationale for screening and treatment of anemia in persons suffering from cardiac or pulmonary symptoms, in order to improve functional capacity and potentially quality of life.

5. Conclusions

The clinical symptoms commonly attributed to anemia are unspecific and highly prevalent in non-anemic and anemic persons alike. Diagnostic work-up in patients with symptoms such as fatigue, lack of energy and concentration, or dyspnea should not primarily focus on anemia. Other possible causes such as depression, heart failure, asthma, and COPD are more likely and should be given more consideration, especially in out-patient settings.

Supplementary Materials

The following supporting information can be downloaded at: https://www.mdpi.com/article/10.3390/jcm12030921/s1, Table S1: Logistic regression models, bivariate analysis. Only estimates for the predictor anemia are shown.(weighted); Table S2: Multivariate logistic regression models with symptoms of anemia as outcome variables (weighted) including the variable iron deficiency instead of the variable anemia (as compared to Table 5).

Author Contributions

Conceptualization, G.W. and A.A.; Designed the study and performed preliminary analyses. S.K.; Performed the main data analysis, S.K., G.W., J.-F.C. and A.A.; Interpreted the data, G.W. and S.K. were major contributors in writing the manuscript and can be considered co-first authors. All authors have read and agreed to the published version of the manuscript.

Funding

This research received no specific grant from any funding agency in the public, commercial, or not-for-profit sectors.

Institutional Review Board Statement

This analysis was conducted using data from the SHIP study. The SHIP study was conducted in accordance with the guidelines of the Declaration of Helsinki and approved by the Ethics Committee of the University Medicine Greifswald (protocol codes BB 39/08, 6/19/2008, and BB106/20, 7/2/2020). Written informed consent was provided by all SHIP-study participants. Data storage is handled according to the data safety and management plan of the Institute for Community Medicine of the University Medicine Greifswald.

Informed Consent Statement

Written informed consent was provided by all subjects on enrollment in the SHIP-study.

Data Availability Statement

Data from the SHIP study are available on reasonable request, in accordance with German law and the data protection concept of the Institute for Community Medicine https://www.fvcm.med.uni-greifswald.de/dd_service/data_use_intro.php.

Acknowledgments

The authors wish to thank Marion Schmidt for proofreading the manuscript.

Conflicts of Interest

The authors declare no conflict of interest.

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Figure 1. Flow chart of study population. SHIP: Study of Health in Pomerania.
Figure 1. Flow chart of study population. SHIP: Study of Health in Pomerania.
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Figure 2. Box plot depiction of continuous hemoglobin levels (g/L) in study subjects according to the presence of the symptoms fatigue, lack of energy, lack of concentration, and dyspnea and weakness (0 = symptom is not present; 1 = symptom is present).
Figure 2. Box plot depiction of continuous hemoglobin levels (g/L) in study subjects according to the presence of the symptoms fatigue, lack of energy, lack of concentration, and dyspnea and weakness (0 = symptom is not present; 1 = symptom is present).
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Figure 3. Bivariate logistic regression models (anemia + second variable) with the outcome fatigue; only the estimates (odds ratios and 95% confidence intervals) of the second variable is shown, (weighted).
Figure 3. Bivariate logistic regression models (anemia + second variable) with the outcome fatigue; only the estimates (odds ratios and 95% confidence intervals) of the second variable is shown, (weighted).
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Figure 4. Bivariate logistic regression models (anemia + second variable) with the outcome lack of energy; only the estimates (odds ratios and 95% confidence intervals) of the second variable is shown (weighted).
Figure 4. Bivariate logistic regression models (anemia + second variable) with the outcome lack of energy; only the estimates (odds ratios and 95% confidence intervals) of the second variable is shown (weighted).
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Figure 5. Bivariate logistic regression models (anemia + second variable) with the outcome lack of concentration; only the estimates (odds ratios and 95% confidence intervals) of the second variable is shown (weighted).
Figure 5. Bivariate logistic regression models (anemia + second variable) with the outcome lack of concentration; only the estimates (odds ratios and 95% confidence intervals) of the second variable is shown (weighted).
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Figure 6. Bivariate logistic regression models (anemia + second variable) with the outcome dyspnea and/or weakness; only estimates (odds ratios and 95% confidence intervals) of the second variable is shown (weighted).
Figure 6. Bivariate logistic regression models (anemia + second variable) with the outcome dyspnea and/or weakness; only estimates (odds ratios and 95% confidence intervals) of the second variable is shown (weighted).
Jcm 12 00921 g006
Table 1. Definitions of diseases according to claims data.
Table 1. Definitions of diseases according to claims data.
DiseaseBilling Diagnosis ICD-10 GMTime Frame and Kind of Diagnosis
at least one relevant and confirmed ICD diagnosis coded as …. prior to the SHIP-2/SHIP-Trend study entrance of the participants
AnemiaD50, D64, D55, D59, D53, D51, D61
  • acute diagnosis within 1 year
Heart FailureI50
  • acute diagnosis within 1 year
  • permanent diagnosis within 5 years
Depression, AnxietyF32, F33, F41, F31, F06, F20, F61, F40, F43, F34, F60
  • acute diagnosis within 1 year
DiabetesE10, E11, E13, E14, E12
  • acute diagnosis within 1 year
  • permanent diagnosis within 5 years
Chronic Kidney DiseaseN18
  • acute diagnosis within 1 year
  • permanent diagnosis within 5 years
HypothyroidismE01, E02, E03
  • acute diagnosis within 1 year
  • permanent diagnosis within 5 years
COPDJ44
  • acute diagnosis within 1 year
  • permanent diagnosis within 5 years
AsthmaJ45
  • acute diagnosis within 1 year
  • permanent diagnosis within 5 years
CancerC0–C96
  • acute or permanent diagnosis within 1 year
Charlson Comorbidity Indexrelevant diagnosis
  • acute or permanent diagnosis within 1 year
ICD: International Classification of Diseases, COPD: chronic obstructive pulmonary disease, SHIP: Study of Health in Pomerania.
Table 2. Medication with fatigue as a possible side effect and their Anatomical Therapeutic Chemical Classification (ATC) according to the guideline ‘fatigue’ by the German Society for General Practice and Family Medicine (DEGAM) [16].
Table 2. Medication with fatigue as a possible side effect and their Anatomical Therapeutic Chemical Classification (ATC) according to the guideline ‘fatigue’ by the German Society for General Practice and Family Medicine (DEGAM) [16].
MedicationATC-CODES
Antineoplastic AgentsL01
Benzodiazepine DerivativesN05CD
AntidepressantsN06A
AntipsychoticsN05A
AntihistamineR06A
Antihypertensives and DiureticsC02, C03
OpioidsN02A
Anti-Parkinson DrugsN04
Table 3. Characteristics of all study participants and participants according to anemia status.
Table 3. Characteristics of all study participants and participants according to anemia status.
All Participants
(N = 5979; 100%)
Participants
with Anemia
(n = 379; 6.3%)
Participants without Anemia
(n = 5600; 93.7%)
Women3149 (52.7)183 (3.06)2966 (49.6)
Age
 20–29327 (5.5)18 (0.3)309 (5.2)
 30–4984 (1.4)1953 (32.7)2037 (34.1)
 50–692519 (42.1)138 (2.3)2381 (39.8)
 >=701096 (18.3)139 (2.3)957 (16.0)
Fatigue 1775 (29.7)128 (2.2)1647 (27.5)
Lack of energy 968 (16.2)81 (1.4)887 (14.8)
Lack of concentration 927 (15.5)70 (1.2)857 (14.3)
Shortness of breath/weakness1727 (28.9)145 (2.4)1582 (26.5)
Iron deficiency
(serum ferritin)
292 (5.0)
(180 missing)
95 (1.6)
(13 missing)
197 (3.4)
(167 missing)
Depression /anxiety
(SHIP-data)
1273 (21.3)
(22 missing)
74 (1.2)
(2 missing)
1199 (20.1)
(20 missing)
Depression / anxiety (claims data) 715 (12.0)45 (0.8)670 (11.2)
Insomnia 1453 (24.3)109 (1.8)1344 (22.5)
Hypertension 569 (9.6)
(30 missing)
16 (0.3)
(3 missing)
553 (9.3)
(27 missing)
Heart failure (claims data)121 (2.0)28 (0.493 (1.6)
Chronic kidney disease (claims data) 165 (2.8)44 (0.8)121 (2.0)
Diabetes (claims data)794 (13.3)94 (1.6)700 (11.7)
Hypothyroidism
(claims data)
375 (6.3)27 (0.5)348 (5.8)
Cancer (claims data)92 (1.5)14 (0.2)78 (1.3)
Asthma (claims data)301 (5.0)20 (0.3)281 (4.7)
COPD (claims data)209 (3.5)28 (0.5)181 (3.0)
Charlson Comorbidity Index (claims data)
 04417 (73.9)216 (3.6)4201 (70.3)
 1951 (15.9)63 (1.0)888 (14.9)
 2324 (5.4)42 (0.7)282 (4.7)
 3–5253 (4.2)49 (0.8)204 (3.4)
 6–934 (0.6)9 (0.2)25 (0.4)
Number of medications
 01656 (27.7)69 (1.2)1587 (26.5)
 11125 (18.8)48 (0.8)1077 (18.0)
 2877 (14.7)40 (0.7)837 (14.0)
 3607 (10.2)37 (0.7)570 (9.5)
 4465 (7.8)29 (0.5)436 (7.3)
 5385 (6.4)37 (0.6)348 (5.8)
 >6864 (14.4)119 (1.9)745 (12.5)
Medication with possible side-effect fatigue 1061 (17.8)112 (1.9)949 (15.9)
Pregnant 199 (3.3)4 (0.1)195 (3.2)
COPD: chronic obstructive pulmonary disease, SHIP: Study of Health in Pomerania.
Table 4. Categorization of anemia severity in anemic study subjects according to hemoglobin normal values from the World Health Organization [15].
Table 4. Categorization of anemia severity in anemic study subjects according to hemoglobin normal values from the World Health Organization [15].
Anemia SeverityWomen
(n = 179)
Pregnant Women
(n = 4)
Men
(n = 196)
Mild110–119 g/L100–109 g/L110–129 g/L
140 (78.4%)4 (100%)179 (92.2%)
Moderate80–109 g/L70–99 g/L80–109 g/L
39 (21.6%)-15 (6.4%)
Severe<80 g/L<70 g/L<80 g/L
--2 (1.4%)
Anemic subjects from the population-based study cohorts SHIP-START-2 and SHIP-TREND were categorized according to WHO normal values for hemoglobin levels in the respective patient groups ‘women’, ‘pregnant women’, and ‘men’. WHO: World Health Organization, SHIP: Study of Health in Pomerania.
Table 5. Multivariate logistic regression models with symptoms of anemia as outcome variables (weighted).
Table 5. Multivariate logistic regression models with symptoms of anemia as outcome variables (weighted).
Outcomes
FatigueLack of EnergyLack of ConcentrationDyspnea and/or Weakness
PredictorsOR (95% CI)
n = 5957
OR (95% CI)
n = 5957
OR (95% CI)
n = 5957
OR (95% CI)
n = 5957
Model 1Model 2Model 1Model 2Model 1Model 2Model 1Model 2
Anemia1.15
(0.94; 1.40)
1.19
(0.98; 1.46)
1.41
(1.09; 1.81)
1.45
(1.13; 1.86)
1.12
(0.87; 1.44)
1.13
(0.88; 1.46)
1.04
(0.85; 1.29)
1.11
(0.90; 1.37)
Women1.40
(1.26; 1.55)
1.42
(1.28; 1.57)
1.33
(1.16; 1.52)
1.33
(1.16; 1.53)
1.12
(0.98; 1.28)
1.11
(0.97; 1.28)
1.08
(0.97; 1.21)
1.09
(0.98; 1.22)
Age (years)0.98
(0.97; 0.99)
0.98
(0.98; 0.99)
0.98
(0.97; 0.99)
0.99
(0.98; 1.00)
1.01
(1.00; 1.01)
1.01
(1.00; 1.02)
1.01
(1.01; 1.02)
1.03
(1.02; 1.04)
Number of medications1.11
(1.08; 1.13)
-1.13
(1.09; 1.16)
-1.08
(1.05; 1.10)
-1.19
(1.17; 1.22)
-
Medication with possible side effect fatigue-1.25
(1.10; 1.42)
-1.58
(1.36; 1.85)
-1.70
(1.47; 1.98)
-1.69
(1.49; 1.92)
Depression and/or anxiety (SHIP)3.44
(3.08; 3.84)
3.49
(3.13; 3.91)
8.22
(7.22; 9.36)
8.13
(7.14; 9.26)
6.79
(5.95; 7.74)
6.58
(5.77; 7.51)
2.66
(2.36; 2.99)
2.68
(2.38; 3.01)
Insomnia (SHIP)2.24
(2.01; 2.49)
2.31
(2.08; 2.57)
2.06
(1.80; 2.35)
2.12
(1.86; 2.43)
1.76
(1.54; 2.02)
1.78
(1.56; 2.04)
1.65
(1.47; 1.84)
1.72
(1.54; 1.93)
CCI (claims data)1.10
(1.04; 1.16)
1.18
(1.12; 1.25)
1.07
(0.99; 1.14)
1.15
(1.08; 1.22)
1.08
(1.01; 1.15)
1.11
(1.04; 1.18)
1.09
(1.03; 1.16)
1.20
(1.14; 1.27)
Heart failure (claims data)------2.66
(1.7; 4.00)
3.03
(2.03; 4.53)
COPD (claims data)------1.99
(1.49; 2.65)
2.14
(1.61; 2.83)
Asthma (claims data)------3.36
(2.67; 4.25)
3.63
(2.88; 4.56)
OR: odds ratio, 95% CI: 95% confidence interval, CCI: Charlson Comorbidity Index, COPD: chronic obstructive pulmonary disease, SHIP: Study of Health in Pomerania. Bold numbers = statistically significant.
Table 6. Number of symptoms in subgroups and positive predictive value of anemia symptoms, weighted percentages.
Table 6. Number of symptoms in subgroups and positive predictive value of anemia symptoms, weighted percentages.
Number of SymptomsAll Participants
(n = 5979) (%)
Participants without Anemia
(n = 5600) (%)
Participants with Anemia
(n = 379) (%)
Positive Predictive Value %
(95% CI)
Four Symptoms295 (4.9)271 (4.7)24 (6.6)8.4 (5.8–10.9)
Three Symptoms430 (7.2)387 (6.9)43 (10.5)8.9 (6.8–11.2)
Two Symptoms708 (11.5)658 (11.4)50 (13.1)6.9 (5.4–8.5)
One Symptom1511 (24.7)1412 (24.7)99 (24.6)6.1 (5.1–7.1)
CI: confidence interval.
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MDPI and ACS Style

Weckmann, G.; Kiel, S.; Chenot, J.-F.; Angelow, A. Association of Anemia with Clinical Symptoms Commonly Attributed to Anemia—Analysis of Two Population-Based Cohorts. J. Clin. Med. 2023, 12, 921. https://doi.org/10.3390/jcm12030921

AMA Style

Weckmann G, Kiel S, Chenot J-F, Angelow A. Association of Anemia with Clinical Symptoms Commonly Attributed to Anemia—Analysis of Two Population-Based Cohorts. Journal of Clinical Medicine. 2023; 12(3):921. https://doi.org/10.3390/jcm12030921

Chicago/Turabian Style

Weckmann, Gesine, Simone Kiel, Jean-François Chenot, and Aniela Angelow. 2023. "Association of Anemia with Clinical Symptoms Commonly Attributed to Anemia—Analysis of Two Population-Based Cohorts" Journal of Clinical Medicine 12, no. 3: 921. https://doi.org/10.3390/jcm12030921

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