Preoperative Predictors of Early Mortality Risk in Isocitrate Dehydrogenase-Wild-Type Glioblastoma Patients Treated with Standard Therapy.

PURPOSE: Early identification of early mortality for glioblastoma (GBM) patients based on laboratory findings at the time of diagnosis could improve the overall survival. The study aimed to explore preoperative factors associated with higher risk of early death (within 1 year after surgery) for isocitrate dehydrogenase (IDH) -wild-type (wt) GBM patients. PATIENTS AND METHODS: We conducted a retrospective analysis of 194 IDH-wt GBM patients who underwent standard treatment. The probability of dying within 1 year after gross total resection (GTR) was defined as the end point "early mortality". Retrospective collection of predictive factors including clinical characteristics and laboratory data at diagnosis.
RESULTS: Median follow-up time after GTR was 16 months (3-41 months). Forty-two patients died within 1 year after surgery (1-year mortality rate: 21.6%). All potential predictive factors were assessed on univariate analyses, which revealed the following factors as associated with higher risk of early death: older age (P = 0.013), occurrence of non-seizures symptoms (P = 0.042), special tumor positions (P = 0.046), higher neutrophil-to-lymphocyte ratio (NLR) (P = 0.015), higher red blood cell distribution width (RDW) (P = 0.019), higher lactate dehydrogenase (LDH) (P = 0.005), and higher fibrinogen (FIB) (P = 0.044). In a multivariate analysis, tumor location (P = 0.012), NLR (P = 0.032) and LDH (P = 0.002) were independent predictors of early mortality. The C-index of the nomogram was 0.795. The calibration curve showed good agreement between prediction by nomogram and actual observation.
CONCLUSION: Tumor location, preoperative elevated NLR and serum LDH level were independent predictors for 1-year mortality after GTR. We indicate that increased preoperative NLR or LDH may guide patients to review head magnetic resonance imaging (MRI) more frequently and regularly to monitor tumor progression.

Introduction

Glioblastoma multiforme (GBM) is the most common and lethal type of cerebral tumor, accounting for 57% of all gliomas and 48% of all primary malignant central nervous system tumors, with the age adjusted average annual incidence of 3.19 per 100 000 individuals.1,2 The incidence associated with progressive decline in neurological function and quality of life can have a devastating impact on patients and their families.3 In 2016, the World Health Organization reclassified the definition of GBM, dividing these tumors into 90% IDH-wt and 10% IDH-mutant GBM. IDH1/2 mutations are rare in GBM and generally carry a better prognosis, while IDH-wt GBM comes to be regarded as a more delineated entity: the most common and malignant astrocytic glioma.4 The first stage treatment for newly diagnosed GBM is maximally safe surgical resection, followed by concurrent chemoradiotherapy and adjuvant therapy with temozolomide. Over the years, with advances in surgical and radio‐chemotherapeutics treatments, the current patient overall median survival has been improved to >15 months.5–7 Noteworthy, the 1-year relative survival rate for patients diagnosed in the United States between 2000 and 2014 was estimated to be only about 41.4%.8 Recently, more and more attention has been paid to the inclusion of predictive factors used for appropriate risk classification into new strategies for cancer therapy in order to improve the survival time of patients with GBM.

Early mortality in GBM patients is associated with various factors. Some GBM patients may die in the short term after surgical resection, mainly due to established adverse factors such as poor performance status, combination of other malignancies, incomplete extent of resection, and lack of adjuvant therapy, rather than the tumor’s own mechanism of action.9–11 In the clinical process, we found that those patients who were in good performance status and received standard treatment could still die unexpectedly within the first year from surgical resection. Therefore, the preoperative identification of those patients is of strong clinical value, as those patients can be timely selected for further radical treatment, clinical trial consideration, and supportive care to improve oncologic outcomes.

Mounting evidence has revealed that preoperative hematological biomarkers, which reflect the tumor microenvironment of the body to a certain extent, could serve as diagnostic and prognostic markers for human cancers.12,13 Previous investigations have indicated that markers of inflammatory response, such as NLR, platelet-to-lymphocyte ratio (PLR), and lymphocyte-to-monocyte ratio (LMR), are associated with the clinical outcomes of gliomas, especially GBM.14,15 Several studies have indicated that a state of preoperative hypercoagulability is related to poor prognosis in patients with GBM.16,17 Other factors such as glucose (GLC), albumin-to-globulin ratio (AGR), the prognostic nutrition index (PNI), LDH and RDW have also been shown to have prognostic value in GBM.18–22

To date, little knowledge is available about the early death rate and preoperative factors related to early death in GBM patients treated with standard therapy. The objective of this study was to explore preoperative predictors associated with higher risk of early mortality (within 1 year after GTR) for IDH-wt GBM patients.

Patients and Methods

Patients

The retrospective study included patients who were newly diagnosed with GBM between June 2016 and August 2019 at the First Affiliated Hospital of Zhengzhou University. Patients meeting the following criteria were included: 1) patients with IDH-wt GBM confirmed by histopathology; 2) patients aged ≥ 18 years; 3) preoperative and postoperative Karnofsky Performance Status (KPS) scores ≥ 70; 4) patients with complete data of routine blood test, coagulation function and hepatic function results; 5) radiotherapy plus concomitant and adjuvant temozolomide were the Stupp regimen; The exclusion criteria were as follows: 1) patients with a clinical history of more than 1 year; 2) patients with midline GBM; 3) patients with obvious infection, autoimmune or hematological diseases; 4) patients with other malignancies; and 5) perioperative surgery-related mortality. A total of 452 patients with GBM were identified from our database, and 194 patients were finally enrolled. All patients enrolling in the current study underwent standard treatment, including GTR, followed by concurrent chemoradiotherapy and adjuvant therapy with temozolomide. No patients received chemotherapy or radiotherapy before the operation. Each patient was followed up regularly until death or October 2020. The patients were observed once every month in the first 6 months after surgery and then every 3–6 months thereafter. The Ethics Committee of the First Affiliated Hospital of Zhengzhou University approved this study and requirement for signed informed consent from patients was waived because of the retrospective nature of the analysis. All patient data were treated with confidentiality, in accordance with the Declaration of Helsinki.

Data Collection

The primary objective was the identification of preoperative predictors of early death, which were defined as death within 1 year after GTR.23,24 As previous studies, a KPS score ≥ 70, which was equivalent to the Eastern Cooperative Oncology Group Performance Status (ECOG PS) score ≥ 1, was considered as the good performance status.25–28 The following variables were collected from hospital case documents: age at diagnosis, sex, first presenting symptoms, clinical history, KPS score, tumor size, tumor location, and laboratory data. Preoperative laboratory markers included: NLR = neutrophil-to-lymphocyte ratio, PLR = platelet-to-lymphocyte ratio, LMR = lymphocyte -to- monocyte ratio, PNI = the albumin value (g/L) + 0.005 × peripheral lymphocyte count/mm3, AGR = albumin-to-globulin ratio, RDW = red blood cell distribution width, GLC = glucose, LDH = lactate dehydrogenase, FIB = fibrinogen levels, and DD = D-dimer levels. Overall survival (OS) as the endpoint was defined as the interval between tumor resection and death or the last date of follow-up. Clinical history referred to the time from onset of symptoms to hospital admission.

Statistical Analysis

Differences in continuous variables were analyzed using the independent sample t-test while categorical variables were evaluated using Chi-squared test or Fisher’s exact test as appropriate. Receiver operating characteristic (ROC) curve analysis was used to determine the optimal cutoff value of each hematological marker according to the area under the ROC curve (AUC). Patients were classified into binary categories according to the cutoff values. Univariable Cox analysis was performed with all patients’ clinical covariates to screen out the factors associated with early mortality. All covariates significant on univariate analysis were included in multivariate Cox analysis. The hazard ratio and P-value of covariates from the Cox analysis were visualized by forest plot. Survival curves were depicted using the Kaplan–Meier method and compared using the Log rank test. A nomogram used to predict the probability of early death was formulated based on the results of multivariate analysis. The performance of the nomogram was measured by C-index and assessed by comparing nomogram-predicted versus observed Kaplan–Meier estimates of survival probability. Decision curve analysis (DCA) was used to evaluate the clinical application of the nomogram. Statistical analyses were performed using SPSS software (version 21.0), and R software (version 3.3.0). P < 0.05 was considered statistically significant.

Results

Patient Characteristics

The clinical characteristics of all patients are shown in Table 1. During the follow-up process, the median OS durations after GTR was 16 months (3‐41 months). Median patient age was 55 years (range 19 to 80), median clinical history was 20 days (range 1 to 365),59.3% of the patients were men, 36.6% had tumor size >5 cm, and 11.4% had seizures as the first presenting symptom. The top three common tumor locations were the mixed lobe location for 69 (35.6%), frontal lobe location for 45 (23.2%), and temporal lobe location for 43 (22.2%), respectively. Median NLR: 2.37 (IQR 1.69–4.19), PLR: 130.04 (IQR 93.42–174.22), LMR: 3.47 (IQR 2.63–4.73), PNI: 50.0 (IQR 47.2–53.6), AGR: 1.75 (IQR 1.53–1.98), RDW: 13.3 (IQR 12.8–13.9), GLC: 4.97 (IQR 4.48–5.75), LDH: 176 (IQR 157–200), FIB: 3.01 (IQR 2.55–3.65), DD: 0.11 (IQR 0.08–0.17). In , we determined the cutoff values of ten hematological factors for OS by ROC curve analysis (NLR‐1.706, PLR‐87.857, LMR‐3.067, PNI‐56.5, AGR‐1.908, RDW-12.8, GLC-6.57, LDH-182, FIB-3.81, DD-0.183). Then, patients were classified into low‐risk and high‐risk groups according to the cutoff points. Table 2 compares the preoperative risk factors of postoperative death within 1 year after GTR. 134 patients (69.1%) died during follow‐up and 42 (21.6%) within 1 year from surgery. One‐year mortality was significantly associated with age, tumor location, NLR, RDW, LDH and FIB.

Table 1

Summary of Clinical Characteristics of GBM Patients Who Received Standard Treatment

Characteristics	All Patients, N = 194
Age, years
Median	55
Range	19–80
Clinical history, days
Median	20
Range	1–365
Sex, n (%)
Male	115(59.3)
Female	79(40.7)
Size, cm, n (%)
≤5	123(63.4)
>5	71(36.6)
First presenting symptoms, n (%)
Seizures	22(11.4)
Others	172(88.6)
Tumor location, n (%)
Frontal	45(23.2)
Temporal	43(22.2)
Mixed	69(35.6)
Others	37(19.1)
NLR, median (IQR)	2.37 (1.69–4.19)
PLR, median (IQR)	130.04 (93.42–174.22)
LMR, median (IQR)	3.47 (2.63–4.73)
PNI, median (IQR)	50.0 (47.2–53.6)
AGR, median (IQR)	1.75 (1.53–1.98)
RDW, %, median (IQR)	13.3 (12.8–13.9)
GLC, mmol/L, median (IQR)	4.97 (4.48–5.75)
LDH, U/L, median (IQR)	176 (157–200)
FIB, g/L, median (IQR)	3.01 (2.55–3.65)
DD, mg/L, median (IQR)	0.11 (0.08–0.17)
OS, months
Median	16
Range	3-41
Survival Status, n (%)
Alive	60(30.9)
Dead	134(69.1)

Abbreviations: NLR, the neutrophil-to-lymphocyte ratio; PLR, the platelet-to-lymphocyte ratio; LMR, the lymphocyte -to- monocyte ratio; PNI, the prognostic nutrition index; AGR, albumin-to-globulin ratio; RDW, red blood cell distribution width; GLC, glucose; LDH, lactate dehydrogenase; FIB, fibrinogen; DD, D-dimer; IQR, interquartile range; OS, overall survival.

Table 2

Comparison of Preoperative Risk Factors for Postoperative Death Within 1 Year After GTR

Characteristics	Death Within 1 Year (42)	Death After 1 Year (152)	P-value
Age, years
Median	56.5	55	0.022
Range	21–80	19–78
Clinical history, days
Median	20	20	0.452
Range	2–365	1–365
Sex, n (%)
Male	25(59.5)	90(59.2)	0.971
Female	17(40.5)	62(40.8)
Size, cm, n (%)
≤5	29(69.0)	94(61.8)	0.391
>5	13(31.0)	58(38.2)
First presenting symptoms, n (%)
Seizures	2(9.1)	20(13.2)	0.213
Others	40(95.2)	132(86.8)
Tumor location, n (%)
Frontal	5(11.9)	40(26.3)	<0.001
Temporal	3(7.1)	40(26.3)
Mixed	29(69.0)	40(26.3)
Others	5(11.9)	32(21.1)
NLR, n (%)
≤1.706	4(9.5)	46(30.3)	0.012
>1.706	38(90.5)	106(69.7)
PLR, n (%)
≤87.857	4(9.5)	36(23.7)	0.073
>87.857	38(90.5)	116(76.3)
LMR, n (%)
≤3.067	11(26.2)	56(36.8)	0.199
>3.067	31(73.8)	96(63.2)
PNI, n (%)
≤56.5	35(83.3)	134(88.2)	0.409
>56.5	7(16.7)	18(11.8)
AGR, n (%)
≤1.908	14(33.3)	47(30.9)	0.766
>1.908	28(66.7)	105(69.1)
RDW, %, n (%)
≤12.8	5(11.9)	47(30.9)	0.014
>12.8	37(88.1)	105(69.1)
GLC, mmol/L, n (%)
≤6.57	32(76.2)	134(88.2)	0.051
>6.57	10(23.8)	18(11.8)
LDH, U/L, n (%)
≤182	16(38.1)	96(63.2)	0.004
>182	26(63.2)	56(36.8)
FIB, g/L, n (%)
≤ 3.81	31(73.8)	132(86.8)	0.041
>3.81	11(26.2)	20(13.2)
DD, mg/L, n (%)
≤0.183	28(66.7)	122(80.3)	0.063
>0.183	14(33.3)	30(19.7)

Abbreviations: NLR, the neutrophil-to-lymphocyte ratio; PLR, the platelet-to-lymphocyte ratio; LMR, the lymphocyte -to- monocyte ratio; PNI, the prognostic nutrition index; AGR, albumin-to-globulin ratio; RDW, red blood cell distribution width; GLC, glucose; LDH, lactate dehydrogenase; FIB, fibrinogen; DD, D-dimer.

Univariate and Multivariate Analyses

In univariate Cox analysis, 7 predictive variables were associated with higher risk of early death within 1 year after GTR: older age (P = 0.013), occurrence of non-seizures symptoms (P = 0.042), special tumor positions (P = 0.046), higher NLR (P = 0.015), higher RDW (P = 0.019), higher LDH (P = 0.005), and higher FIB (P = 0.044) (Figure 1A). The predictive performance of all significant characteristics was assessed using the AUCs obtained from ROC curves. According to the AUCs, LDH was the leading factor for predicting early death, which showed its significant predictive potential (0.625 vs 0.565 to 0.615; Figure 2). In multivariate Cox analysis, tumor location (HR = 1.590, 95% CI 1.107‐2.284; P = 0.012), NLR (HR = 3.164, 95% CI 1.107‐9.041; P = 0.032) and LDH (HR = 2.580, 95% CI 2.875‐5.528; P = 0.002) remained independently associated with 1‐year mortality after GTR (Figure 1B).

Figure 1

Preoperative predictive factors for 1‐year mortality after GTR according to COX regression.

Figure 2

Receiver operating characteristic (ROC) curves of significant clinical covariates for overall survival.

Survival Analysis of Independent Predictive Hematological Markers

As shown in Figure 3A, GBM patients with NLR > 1.706 showed a significantly poorer OS than that of GBM patients with NLR ≤ 1.706 (P = 0.009). Similarly, the OS of patients in the LDH high-risk group was significantly lower than that of patients in the LDH low-risk group (P = 0.004, Figure 3B). The results indicated that preoperative NLR and LDH level may be used in clinical practice to identify high-risk patients.

Figure 3

Comparison of survival curves of GBM patients at different hematological groups.

Development of the Nomogram Related to Early Death

The prognostic nomogram that integrated all significant factors for early death in multivariate Cox regression analysis is shown in Figure 4A. Every covariate was allocated a score based on the multivariate Cox analysis, and the nomogram score termed total points was generated by summing risk points scores of all the covariates. Tumor location had maximum score points (ranging from 25 to 100) compared to other clinical factors. Among them, mixed lobe location had higher risk scores for early mortality compared with patients with tumor located in other positions. The C-index of the nomogram for early mortality prediction was 0.795. The calibration plot for the probability of survival at 1 year after GTR showed an optimal agreement between the prediction by nomogram and actual observation (Figure 4B). The results of DCA showed that the nomogram could yield clinical net benefits (Figure 4C).

Figure 4

Establish an overall survival nomogram to predict the probability of early death in GBM.

Discussion

In recent decades, despite continuous improvements in neurosurgery techniques and innovations in new treatment methods, such as immunotherapy and molecular-targeted therapy, the survival time of patients with GBM is still not optimistic.2,29,30 It is noteworthy that a certain number of GBM patients with good preoperative and postoperative health status, who received standard treatment protocols, should have better clinical outcomes, but instead had an endpoint event ie, death within 1 year. Thus, we focused on IDH-wt GBM patients with preoperative and postoperative KPS scores ≥70 (ECOG PS scores ≥ 1) and receiving standard treatment including GTR, followed by concurrent chemoradiotherapy and adjuvant temozolomide. In addition, accumulating studies have demonstrated that peripheral blood test parameters play a remarkable role in the prognosis of various malignant tumors, such as lung cancer, gastric cancer, and soft tissue sarcoma, as well as GBM.31–33 Unlike genetic biomarkers, preoperative hematological markers, which are detected via noninvasive procedures and are more cost-effective, can be easily obtained from routine blood tests. In the present study, we included 194 homogenous IDH-wt GBM patients to assess preoperative risk factors for early death. Further, we collected all hematological indicators of these patients that have been proven to be prognostic in previous studies, and incorporated them into subsequent analyses as binary variables based on the ROC curve. Multivariable analyses identified the following three factors as predictive of early death: tumor location, preoperative NLR and serum LDH level. To further improve the accuracy of the prediction of early mortality, we established a nomogram based on clinical and hematological parameters. The C-index of the nomogram was 0.795, which showed excellent predictive power. This may guide the neurosurgeons in early identification of GBM patients with a high probability of early mortality before surgery, so as to instruct these high-risk patients to review head MRI more frequently and regularly, and to increase follow-up of these patients.

In the present study, tumor location had a significant effect on the occurrence of early death. GBM patients with tumors located in mixed areas had higher risk for early mortality than those with tumors located in the frontal and temporal lobes. In addition, tumor location was the dominant factor compared to other clinical factors in the nomogram. The prognostic role of tumor location for patients with GBM has been evaluated by previous investigations.34 A recent publication by Dietterle et al revealed that the hazard ratio of unilobar tumors is twice that of multilobar tumors.35 Tumors located in mixed areas are adjacent to many critical arteriovenous structures and functional areas. Therefore, tumors located in these regions may increase the difficulty of operative and incidence of complications, which could result in early mortality and unfavorable long-term clinical outcomes.

The effect of NLR on early mortality was also apparent in our study results. We demonstrated that patients with high-NLR have worse OS compared with low-NLR patients undergoing GTR. Recently, there has also been considerable evidence that inflammation is closely related to the occurrence and development of malignant tumors, the concept of cancer-related inflammation has also been proposed.12 Some inflammatory parameters are associated with adverse prognostic outcomes of gliomas, the most representative of which is NLR.36 Published qualitative results have shown that neutrophil can promote the progression of glioma by remodeling the extracellular matrix and promoting angiogenesis, and that certain subsets of T-lymphocytes can instead inhibit it via induction of cytotoxic cell death and cytokine production.12,37 Accordingly, high neutrophil and low T-cell (elevated NLR) in GBM was correlated with poorer outcome.15,38 However, the predictive value of NLR for early death has not yet been reported in GBM patients receiving standard treatment. We believe that preoperative NLR might represent cancer-related systemic inflammation response to evaluate the early mortality of GBM.

In our study, we also further observed that preoperative serum LDH level is significantly associated with 1‐year mortality. LDH is released from cells upon damage to their cytoplasmic membrane, and is both a metabolic and an immune surveillance prognostic biomarker. Increased LDH level is a negative prognostic biomarker, not only because it is a key enzyme involved in tumor metabolism, but also because it allows cancer cells to suppress and evade the immune system by altering the tumor microenvironment.39–41 To the best of our knowledge, the relationship between preoperative LDH level and early mortality in GBM patients has not yet been investigated. The present findings suggested that serum LDH level might serve as a preoperative predictive factor to identify early death of GBM patients.

However, some limitations of the present study should be considered. First, this was a single-center retrospective study that may have led to bias in selection and analysis. Second, since the values of the hematological markers were entered into Cox regression as categorical variables, the optimal cutoff value needs to be further verified in future studies. Finally, the number of patients is somewhat small to make a final conclusion on this matter. Considering the limited number of the study conducted, further studies are needed to identify and characterize of the GBM patients with a high probability of early mortality.

Conclusion

In summary, tumor location, NLR, and serum LDH level are independent predictors for 1‐year mortality after standard treatment. To the best of our knowledge, this is the first study to investigate the predictive value of preoperative NLR and serum LDH level for early death in GBM patients with standard therapy. Following the results, increased preoperative LDH or NLR should lead to more frequent and regular head MRI reviews to monitor tumor progression.