RETRACTED ARTICLE: Investigations of renal function using the level of neutrophil gelatinase-associated lipocalin associated with single-dose of cisplatin during chemotherapy

Cisplatin (CP) found in the 1960s to inhibit cell division, is currently one of the most widely used anticancer chemotherapy drugs [1, 2]. CP is mainly used for different kind of cancer including head and neck cancer, esophageal cancer, genital cancer (i.e., testicular and ovarian cancer), cervical cancer, and non-small-cell lung cancer [3, 4], and its adverse clinical effects, including neurotoxicity, ototoxicity, nephrotoxicity, nausea, and vomiting, remain challenging for clinicians [1‐3]. Clinically, CP-induced AKI occurs about 10 days after CP treatment, and it is marked by a decline in glomerular filtration rates, increased serum creatinine levels, hypomagnesaemia, and hypokalemia [2, 4, 5]. Due to the high blood flow through the renal relative to its mass and subsequent exposure to concentrated urine including omitted xenobiotics the renal is one of the known main signal tissues for medication-induced injury [6]. Although clinicians have exerted efforts to prevent CP-induced AKI, the results are not satisfactory. A biomarker that predicts AKI earlier than serum creatinine levels may provide clinicians with more time to apply the appropriate intervention [6, 7].

Recent studies have investigated some biomarkers, including NGAL, which is a 25-kDa protein. This biomarker is known as an primary indicator of acute and chronic renal trauma [7‐14]. Low concentration of NGAL is present in most human tissues but spikes when kidney, liver, colon, and lung epithelial cells are damaged. Recently, there are a number of studies that suggested serum and urine NGAL are sensitive and specific biomarkers for the prediction of AKI as well as the development of AKI among human patients after cardiac surgery [15], non-cardiac surgery [16], and renal transplantation. It has been reported that the expressions of NGAL are rapidly up-regulated after renal injury and is highly expressed during ischemic renal injury in animal models. It is worth noting that researches on animal model have shown, which NGAL levels increase after ischemic kidney injury or exposure to nephrotoxic drugs [17‐21].

In veterinary medicine, NGAL is a newly studied and promising biomarker that has been shown to increase in dogs with both AKI and chronic kidney disease (CKD). NGAL was shown to be a sensitive biomarker for AKI in dogs undergoing different types of surgeries and experimentally in a canine model of gentamicin nephrotoxicity [22].

In an animal study, urinary NGAL levels that were measured by western blots were increased within 3 h after CP treatment in an AKI study group [21]. In reply to multifarious kinds of damage, elicitation of multiple of this indicator is known to elevate, and they may be distributed or energetically discharged into the urine or blood flow [14]. Furthermore, it has been reported that NGAL synthesis is also increased in cancer.

The aim of this study was to evaluate serum and urinary biomarker including NGAL (sNGAL and uNGAL) in canine with solid renal tumors who suffered from CP after short and long-term chemotherapy.

NGAL is a 25-kDa protein which is known as a primary indicator of acute and chronic renal trauma [14, 15]. It has been reported that the expressions of NGAL are rapidly up-regulated after renal injury in animal. It is worth noting that research on animal model have shown, which NGAL levels increase after ischemic kidney injury or exposure to nephrotoxic drugs. Use of NGAL as a marker in dogs with naturally occurring kidney disease has only recently been explored in AKI [22].

In an animal study, urinary NGAL levels that were measured by western blots were increased within 3 h after CP treatment in an AKI study group [21]. In reply to multifarious kinds of damage, elicitation of multiple of this indicator is known to elevate, and they may be distributed or energetically discharged into the urine or blood flow [14]. Furthermore, NGAL synthesis is also increased in cancer.

Recently, much attention has been given to NGAL in veterinary nephrology but, there are no studies that plasma and urinary NGAL as a biomarker of CP drug induced ACRI in dogs with kidney cancer. This article focuses on the biomarker NGAL and its potential utility in the pathologic diagnosis, primary prognosis of destruction, and treatment of ACRI.

Our finding showed that the higher concentrations of serum, sNGAL and uNGAL compared with control group (P = 0.024; P = 0.011, Table 2). Indeed, CKI was associated with higher levels of sNGAL and uNGAL compared with exposed controls. Other preliminary investigations have shown elevated serum and urine NGAL concentrations in dogs with kidney diseases compared to controls [21].

The results of this study indicated that NGAL is a promising renal biomarker when serum and urine NGAL concentrations in CP treatment in CKI study group. However, sNGAL can have from different origins and release is not limited to the kidneys, concurrent diseases may contribute to the increase in sNGAL and this might lead to prediction of a poor prognosis.

It has been reported that chemotherapy with CP especially on the animal model, multifarious definitions of acute and chronic renal injuries (ACRI) different settings of ACRI [23‐26].

It has been previously reported which NGAL levels increase after ischemic kidney injury or exposure to nephrotoxic drugs in animal model, For instance, after CP-induced ACRI in mice, [13, 15] and also after acute and chronic renal injuries in mice and rat models. It is worth noting that detectable level of NGAL were observed an hour after onset of injury, which precedes the urinary appearance of beta-2 microglobulin and many other markers of tubular injury [13]. It has been reported that injury in proximal ducts in the renal cortex is mainly occurred due to CP. In addition, the severity of acute renal injury was extremely impressive in proximal tubules [26], which it is in accordance with our finding. It is worth noting that another study indicated that CP could cause extensive damage in renal cortex [27].

The present study indicated that uNGAL is a major biomarker in comparison with sNGAL for the early risk stratification of CKI after CP chemotherapy and is can be as prognostic factor for the early detection of kidney injuries. The median uNGAL concentration at baseline was significantly higher in dogs . Furthermore, at the several studies have been exhibited that U-NGAL excretion predicted ACRI in patients with solid tumors such as renal cancers receiving CP, which is in agreement with our study. However, another study have been reported which U-NGAL levels predicted ACRI in a multicenter cohort of children with diarrhea-associated hemolytic uremic syndrome [28‐32]. In parallel, the highest level of uNGAL was seen in comparison with sNGAL, after a high dose administration of CP. This result is in agreement with the finding previous report that suggested the urinary NGAL as a marker of tubular damage depends on these parameters [33].

Together taken, NGAL concentrations in urine and in serum can be used clinically in dogs as biomarkers to evaluate renal function. To the authors’ knowledge, this is the first study that suggested that urinary and plasma NGAL excretion after CP chemotherapy in dog with CKI.

Current study indicated that U-NGAL may be as effective marker to monitor renal injury in exposed CKI patients to CP. Furthermore, a primary elevate in urinary NGAL expulsion may help in identifying cases at danger of CP-induced CKI that might profit from innovative remedies to prevent CP nephrotoxicity. Further studies are required to determine the true predictive and prognostic value of NGAL for dogs with solid renal cancer treated with CP.