Hemoglobin concentration; a pathway to frailty

Frailty is a geriatric syndrome, prevalent in old age leading to an increased risk of negative health outcomes such as morbidity, mortality [1] and appears to be a transitional state in a dynamic process from robustness to disability [2]. It is defined as a state of increased vulnerability to stressors resulting from age-related decline in physiological reserve [3].

As a clinical condition, it is characterized by the presence of more than three of the five Fried criteria (intentional weight loss, self-reported exhaustion, weakness, slow walking speed and low physical activity [4]) and is based on the relationship between biological and age associated markers linked in a cycle of frailty.

With demographic changes in society such as population aging, prevention of disability has risen to the fore of medical and economic concerns. Despite research and publications, mechanisms of frailty development remain poorly understood [5]

Anemia and frailty are two common findings in geriatric patients and have been shown to be associated with similar poor health outcomes [6]. Anemia leads to diminished tissue oxygenation which may provoke diverse symptoms such as fatigue, weakness, and increased physical impairment. The symptoms of anemia are highly correlated with the symptoms associated to frailty and therefore may highlight a relationship between hemoglobin count and frailty [7, 8].

While the criteria as set out by the World Health Organization (WHO) are universally accepted, further study of anemia and frailty are frustrated by the continued debate of the cut off values chosen to define anemia in older populations [9, 10]. Certain studies have shown that lower hemoglobin count, above what would be considered clinical anemia predicts negative health outcomes such as mortality, morbidity and low physical performance [10‐12]. As such there is growing evidence that lower hemoglobin concentration is associated to frailty given their high prevalence together in an older population and their common health outcomes [13]. Whether low hemoglobin results in a state of frailty or vice versa, or are the symptoms of a common physiological state is yet to be investigated.

The close relationship between lower hemoglobin concentration and the definition of frailty suggests that lower hemoglobin concentration could be a stepping stone in explaining the frailty syndrome. Cecchi et al. show in their study that lower hemoglobin concentration is associated with the decline of self reported physical activity and muscular strength which are potential correlates of frailty [11].

However, whether this association is independent from increased prevalence of comorbidity, causing both low hemoglobin and reduced physical function is under debate. There are a few studies to this day on physiological mechanisms between hemoglobin concentration and frailty [6, 13, 14]. Frailty may be caused by the influence of a range of variables: sociodemographic, physical, biological, lifestyle and psychological factors [15]. Certain of these variables share a common influence on hemoglobin concentration such as nutritional deficiency, chronic renal failure and chronic inflammation [16].

Identifying the respective role of these potential confounders is necessary to study the linkages that exist in the relationship between frailty and hemoglobin concentration.

An important remaining issue is to disentangle common and separate pathways by which both nutritional and inflammation mechanisms can influence this relationship [16, 17].

This study aims to examine the pathways linking hemoglobin concentration to the presence of a frailty syndrome. Our objective was to evaluate whether hemoglobin concentration was an independent predictor of frailty and investigate possibe causal pathways, in particuliar the relationship between inflammation and nutrition with hemoglobin concentration.

Patients who underwent comprehensive geriatric assessment and had a blood draw were assessed for eligibility (n = 1905). The flow chart corresponding to the sample selection used for this study is presented in Fig. 1. A total of 76 patients were excluded: 70 patients due to lack of data on hemoglobine or frailty status and 6 because they had aberrant biological results.

At baseline, the mean age of the participants included in the study was 82.4 years (±6.5), 32.64% were male, and 38.87% completed at least high school (Table 1).

The most-common diseases was hypertension 52.05%. Most of the patients did not have organ insufficiencies nor history of inflammatory diseases and 18.43% of the subjects had a history of cancer. Hemoglobin concentrations ranged from 7.8 g/dl to 17.6 g/dl with a mean 13.33 g/dl (±1.41).

Based on the WHO criteria for anemia, 20.83% of participants were anemic at enrollement. 51.18% of the participants were non frail and were relatively autonomous with a mean score on the activities of daily living scale (ADL) of 5(±1) and on the instrumental activities of daily living scale (IADL) of 5(±2) [32].

Table 2 presents the results of multivariate logistic regression analysis conducted to study the relationship between hemoglobin and frailty.

The crude odds ratio (OR) between hemoglobin and frailty was 0.78 (95%CI 0.72–0.85) This OR of being frail decreased by 22% for an increase of hemoglobin of 1 g/dl after adjustment for gender and age (model 1), as after inclusion of kidney function (OR = 0.79, 95%CI = 0.73–0.86) (model 2). This link persisted after the inclusion in the model of inflammation (OR = 0.81, 95%CI = 0.75–0.89) (model 3), cognition (OR = 0.82, 95%CI = 0.75–0.89) (model 4), nutritional status (OR = 0.86, 95%CI = 0.79–0.94) (model 5) and socio economoic variables (OR = 0.86, 95%CI = 0.79–0.94) (model 6).

Regarding the other determinants of frailty, the risk of being frail increased according to the stage of kidney disease, but this association was not statistically significative.

Inflammation was associated with a 125% risk of being frail (model 3) and this link persisted after inclusion of cognition (OR = 2.26, 95%CI = 1.58–3.25) (model 4) as with the addition of nutritional status (OR = 2.11, 95%CI = 1.45–3.07) (model 5). The risk of being frail increased according to the degree of severity of the cognitive state (model 4). For example the risk of being frail was 4.29 times more higher in the severly impaired (OR = 4.29, 95%CI = 1.60–11.51). This risk was significantly attenuated once adding nutritional status (OR = 1.98, 95%CI = 0.71–5.51) and socio economic variables (OR = 1.72, 95%CI = 0.62–4.81).

Nutritional status was independantly associated with being frail (model 5). The risk of being frail was multiplied by 8 if the patient was in a state of malnutrition.

Education level was independently associated with being frail, the higher the level of education was, decreased the risk of being frail (model 6).

This study examines the influence of hemoglobin concentration on the subsequent risk of being frail after adjustment for a large range of confounders.

This association remained significant after adjusting for age, gender, kidney function, inflammation, cognition, nutritional status and socio-economic position. The results of this study confirm results found in Corona et al. and Juarez-Cedillo et al.’s study but with a wider and older population sample [6, 13]. Moreover, the decision to expand the number of variables under consideration in this study to include kidney function, inflammation, cognition, nutritional status and socio economic variables as they have been identified as potential confounders to frailty and hemoglobin concentration allows a more thorough understanding of this relationship. Thus, they should be adapted in future studies to further assess the causal relationship between these factors.

Looking at the relationship between hemoglobin concentration and disability, Chaves and al. have questionned the clinical appropriateness of the definition of anemia set by the WHO hemoglobin level < 12 g/l for women and < 13 g/l for men [33] given the independent adverse effects of low hemoglobin on mobility function [34]

This seems to be confirmed by the independent association between hemoglobin concentration and frailty status found in our study. Indeed low hemoglobin puts older adults at risk of poor oxygen delivery with exhaustion, fatigue and failing muscle strength [33, 35] Symptoms which are each individual criteria in the definition of frailty by Fried [4].

This hypothesis highlights another issue, which are the mechanisms at stake in lowering hemoglobin concentration.

This was our second objective, studying potential confounders between hemoglobin and frailty. Among all these factors identified: kidney function, inflammation, cognition, nutritional status and socio-economic factors there was no impact on the effect of hemoglobin on frailty after adjustment. This suggests that the relationship between hemoglobin concentration and frailty is independent of these variables and that further studies are required to identify the potential links between them.

Our hypothesis was that lower hemoglobin concentration and frailty are associated to a state of chronic inflammation. Indeed, frail older adults have often a poorer health status, chronic conditions and comorbidites leading to an active low grade of inflammation lowering hemoglobin concentration [36, 37]. However, Walston et al. have provided evidence supporting an activation of inflammation with and without clinical comorbidities, suggesting that there is a direct relationship between frailty and inflammation [36]. Many studies have explored multiple inflammatory biomediators as potential mechanisms by which inflammation might promote lower hemoglobin [17, 38].

We chose in our study CRP as an inflammatory biomediator, after adding CRP in model 3 there was no impact on hemoglobin’s odds ratio (OR = 0.81, IC95%0.75–0.89 p < 0.005) and after studying the interaction between those two parameters the association was not significative (p = 0.14). The lack of relationship might be due to the cut off values used to define inflammation, or the inflammatory biomediator chosen [37, 39]. The pathogenesis of frailty and the role of inflammation remains incompletely understood. Leng et al.’s studied the potential role of neutrophils and monocytes in the pathogenesis of frailty as well as the role of interleukin-6 [14, 39]. There is a probable link between inflammation and frailty, our hypothesis was that maybe lower hemoglobin reflected this effect and could be a mediating factor we could follow to study this relationship. The question is if hemoglobin is a stigma of this relationship between inflammation and frailty or is it an independent actor in the frailty process.

We also studied the relationship between hemoglobin and nutritional status. Low hemoglobin count could be attributed to nutrient deficiencies (Iron, B12 and folate) [16], we kept in light this information and used the MNA [27] score as a proxy of the patient’s nutritional state. Indeed, a patient with malnutrition is more likely to have nutrient deficiencies.

In our study, the risk of being frail increases according to their nutritional status in a bivariate analysis. However, the interaction between frailty, hemoglobine and nutritional status was not significative in this study.

The absence of link between nutritional status and hemoglobine is possibly explained by two hypotheses.

One hypothesis is that nutritional status as determined by the MNA score does not define vitamin deficiency, as patients with vitamin deficiencies are not necessarily malnourished and vice versa [40]. Another hypothesis is that the MNA is a certain type of nutrition screening tool and thus might not identify all situations of malnutrition in the elderly [41].

The main strength of this study is that data was prospectively measured with a large number of participants who underwent a comprehensive frailty assessment and that we used an explanatory model with series of logistic regression taking into account numerous potential confounders.

There are also a number of limitations that need to be considered.

Firstly, we took in account the major confounding factors of hemoglobin concentration, we did not investigate thouroughly all the causes of low hemoglobin concentration as this would have exceeded the purpose of our study.

Secondly, this is a monocentric study, all the study participants have been recruited through the Toulouse frailty day hospital. This may induce a selection and a representativeness bias.

Moreover, participants were referred by a physician (general practitioner, geriatrician or specialist) who had reported signs or symptoms of using the gerontopôle frailty screening tool (GFST) [18], so our findings might be difficultly extended to a general community-dwelling elderly population.

Finally, the cross-sectional nature of our study is the main limitation, a longitudinal analysis may shed light on the chronological and possible etiological relationship between hemoglobin and frailty.

Hemoglobin concentration is strongly associated with frailty in older adults. Addition of different covariates did not influence this relationship and the mechanisms involved in this relationship remain unclear. If hemoglobin concentration is an independent and a causal factor of frailty, improving concentrations of hemoglobin could potentially diminish the risk of frailty and thus detecting low hemoglobin above the score of anemia would be relevant.

Potential pathways linking hemoglobin to frailty deserve further investigations. These results can have potentially important implications for prevention policies targeting frailty, by identifying potential patients with high risk of adverse outcomes and functional outcomes.