Negative association between free triiodothyronine level and contrast-induced acute kidney injury in patients undergoing primary percutaneous coronary intervention

Contrast-induced acute kidney injury (CI-AKI) is a frequent complication after percutaneous coronary intervention (PCI), which is the third most common cause of acute kidney injury in hospitalized patients [1] and is strongly associated with the risk of dialysis, mortality, length of stay and costs [2, 3].Thus, timely identifying patients at high risk of CI-AKI and taking early prophylactic measures are critical.

Thyroid hormones has been generally considered to be associated with kidney for several years, which involved in the growth, development and electrolyte balance maintenance of the kidney [4‐6]. Previous studies have found that the deterioration of renal function is followed by changes in the synthesis, secretion, metabolism and elimination of thyroid hormones [4, 7]. Nonthyroidal illness syndrome (NTIS) is a common manifestation in critically ill patients (including severe cardiac disease and kidney disease) without pre-existing thyroid disease. A decrease in total serum triiodothyronine (T3) and free triiodothyronine (FT3) without elevation of thyroid-stimulating hormone (TSH) is the most common form of NTIS, which was known as low T3 syndrome [8, 9]. Low f3 levels have been reported to be independent predictors of mortality in patients with myocardial infarction [10, 11] or kidney disease [12]. However, it is uncertain whether low FT3 level is related to CI-AKI in patients with ST-elevation myocardial infarction (STEMI) undergoing primary percutaneous coronary intervention (pPCI). Therefore, we aimed to focus on the relationship between low FT3 and CI-AKI in patients undergoing pPCI, and discuss the impact of low FT3 on short and long-term mortality.

The relationship between low T3 syndrome or thyroid dysfunction and AKI has been reported previously [17, 18], yet the relationship between low FT3 and CI-AKI has rarely been investigated. In this study we found that a serum FT3<3.1 pmol/L was an independent risk factor of CI-AKI, as well as a predictor of long-term mortality after pPCI.

The incidence of CI-AKI after pPCI ranges from 11.9 to 17.1% according to previous studies, which is significantly higher than that of elective PCI [19‐23]. As with above studies, our study also demonstrated a similar high incidence of 15% in this population, which is strongly associated with blood volume insufficiency, hemodynamic instability and inadequate hydration. Meanwhile, CI-AKI has been considered to be associated with a poor prognosis. Thus it’s crucial to screen the risk factors of CI-AKI in these patients and to initiate early preventive measures.

Previous studies had identified several risk factors for predicting CI-AKI after pPCI, such as pre-existing renal impairment, advanced age, high contrast medium volume use of intra-aortic balloon pump (IABP), peri-procedural hypotension, and hyperuricemia [16, 19, 23‐26], part of which were also identified as risk factors of CI-AKI in our study. Furthermore, we also found low FT3 was a novel risk factor of CI-AKI after pPCI.

Low FT3 levels are common in patients with chronic kidney disease (CKD). According to the study by Kaptein et al. [7], low FT3 occured in 66% of the 287 euthyroid patients with end-stage renal disease (eGFR< 15 mL/min·1.73 m²). In addition, Sang Heon Song et al. [27] demonstrated the increasing incidence of low T3 along with the increase of CKD stage, even after adjusting for confounders, eGFR remained positively related to T3 levels. There are also growing evidence suggesting low FT3 exerts dramatic effects upon kidney function in various aspects. A more recent study [28] including 2180 euthyroid participants revealed that serum FT3 levels were positively related to both eGFR and creatinine clearance (CrCl) but fT4 and TSH had no significant correlation with either eGFR or CrCl. In an another study [29], the incidence of low FT3 was 71.7% in 669 dialysis patients, low T3 is not only closely associated with CKD but also significantly increases the risk of poor outcomes in CKD patients, furthermore, low FT3 was found to be an independent predictor of cardiovascular mortality (HR = 1.75,95%CI: 1.19–2.57, p = 0.005) in hemodialysis patients during a mean follow-up period of 34 ± 16 months. A cohort study [30] including 114 dialysis patients reinforced that patients with low FT3 had higher risk of all-cause mortality and a shorter survival time than the patients with normal FT3. Although above findings provided a comprehensive view that low FT3 was associated with CKD and was a significant predictor for mortality.

Several studies have also suggested that thyroid function disorders including low FT3 are correlated to AKI. In a prospective study by Iglesias P et al. [17] which enrolled 35 consecutive patients with AKI, alteration in thyroid function tests was detected in over 80% of these patients and the most common disorder was low T3 syndrome. However, due to its short follow-up period and small sample size, this study failed to determine the prognostic value of thyroid function tests for AKI. Another study by Zhang D et al. [18] including 1339 patients in the general intensive care units demonstrated that when Cystatin C (Cys C) was used for detecting early AKI, FT3 was found to be independently associated with Cys C. Furthermore, FT3 had no significant impact on the diagnostic and predictive accuracy of Cys C in detecting AKI in ICU patients. A more recent study by us firstly investigated the relationship between FT3 concentration and CI-AKI in patients aged > 75 years undergoing PCI, which showed the incidence of CI-AKI was about 1.4 folds higher in patients with low FT3 compared with normal FT3, suggesting low FT3 might be a novel risk factor for CI-AKI [31]. It’s well-known that low FT3 is more frequent in critical ill patients such as myocardial infarction. However, the relationship between FT3 and CI-AKI in patients undergoing pPCI is unclear, our findings of the present study fills the gap by demonstrating that FT3 < 3.1 pmol/L was a powerful predictor for CI-AKI in patients after pPCI, even after adjusting for potential confounding factors.

The underlying mechanism has not yet been fully elucidated, several plausible explanations are stated as follows. First, as stated above, low FT3 may be an marker reflecting severe cardiac damage, in which extensive cardiac damage had greater impairment of cardiac function, further declining cardiac output and reducing renal blood flow, and deteriorated renal function [32]. Second, low FT3 level was also considered to be a maladaptive neurohumoral alteration during acute ill condition, for that lower FT3 level contributed to the preservation of energy yet in turn weakened the regeneration and self-repair capability of tubular epithelium [29, 33]. Third, previous studies confirmed that low FT3 directly led to the contraction of renal artery through impaired endothelial function in vitro and in vivo, and deteriorated kidney function [34, 35]. Finaly, the decline of FT3 levels may be caused by decreased conversion of the prohormone T4 into T3 and by increased T3 catabolism, they were associated with hypoxia, inflammation, and oxidative stress, which also be involved in the process of CI-AKI [36‐38].

A low FT3 level is also a common phenomenon reflecting severe cardiac damage and impairment of cardiac function, so that increasing the risk of mortality and other poor outcomes. A recent meta-analysis [39] including 41 studies showed that the incidence of low FT3 in patients with acute myocardial infarction up to 18.9%. Another retrospective study [10] including 501 STEMI patients in China found a even higher rate (34.1%) of low FT3 levels in AMI patients, the low FT3 group had a higher serum levels of TnT, NT-ProBNP, and higher percentage of three diseased vessels, which indicate more serious myocardial injury, furthermore, a low FT3 level was found to be independently associated with short-and long-term death and MACE. Another more recent study by Y Song et al. [11] in 699 consecutive STEMI patients also found that low FT3 levels were independently associated with 30-day and 1-year all-cause death and MACE. Conversely, another prospective study [40] include 457 STEMI patients undergoing pPCI showed that serum FT3 levels were associated with in-hospital MACE and long-term MACE only in univariate analysis but not in multivariate analysis, however, in this study the relationship among risk factors and long-term MACE were analyzed by multivariate logistic regression analyses but not cox regression analyses, which does not consider the time-event factor. In our study, poor prognosis for long-term mortality in STEMI patients with low FT3 undergoing pPCI was also observed. Compared with patients with normal FT3, patients with low FT3 had significantly higher incidence of long-term mortality during 20 months of follow-up (HR = 2.54, 95%CI:1.15–5.60, p < 0.05).

Our study also has several limitations. First, due to the single-center, retrospective nature of this study and the small population included, there may be residual confounding by unmeasured factors. Second, since some parameters were not routinely tested in our hospital, we failed to quantify these parameters including serum reverse T3 in our study. Third, there is a possibility that the true incidence of CI-AKI may have been underestimated in clinical practice due to the potential loss of real peak SCR levels which is restrained by measurement times. Fourth, we failed to explored the optimal cutoff of fT3 concentration for predicting CI-AKI and mortality. Finally, it’s unable to explored the causal correlation between low fT3 and CI-AKI due to the retrospective design of this study, whether this association only simply reflects the severity of the disease of this population was beyond explanation.

In summary, The study showed that serum concentration FT3 < 3.1 pmol/L was an independent risk factor for CI-AKI and long-term mortality in patients undergoing pPCI. Measurement of serum FT3 may help identify patients who were at high risk of CI-AKI and mortality after pPCI.