Background
Cancer is the leading cause of death in the world. Non-small cell lung cancer (NSCLC) is one of the most aggressive diseases and has a poor prognosis compared with other malignancies. NSCLC patients are usually diagnosed at an advanced stage and usually receive chemotherapy. The prognosis of advanced NSCLC patients is improving due to the developments in chemotherapy, and better control of adverse events and complications is becoming more important.
An association between cancer and thrombotic events was first reported by Trousseau in 1865 [
1]. The association between cancer and thrombotic disease including cerebral infarction (CI) is referred to as Trousseau syndrome. Patients with solid tumors, including lung, breast, ovary and pancreas cancers, have significantly higher risk of thromboembolic complications than patients with hematologic malignancies such as leukemia and malignant lymphoma [
2]. In another report, the prevalence of cancer was higher in stroke patients than in the general population (
p = 0.001). The most common cancer types were colorectal cancer (20.2 %), prostate cancer (15.6 %), breast cancer (12.7 %), cancer of the urinary tract system (10.3 %), gynecological cancer (6.2 %) and lung cancer (4.5 %) [
3].
CI impairs activities of daily living and performance status (PS). Most patients with CI will not be able to continue anticancer treatment. Therefore, the survival of cancer patients with CI is poor.
Although some previous papers reported the incidence of CI in lung cancer patients, the incidence rate was based on data from a registry including all lung cancer patients, from early stage to advanced stage [
4,
5]. Moreover, the effect of CI on the prognosis of advanced NSCLC patients has not been reported. The aim of this study was to investigate the association between CI and advanced or post-operative recurrent NSCLC, risk factors for CI in advanced NSCLC, and the effect of CI on the prognosis of advanced NSCLC.
Methods
Study design
Between April 2009 and March 2014, 532 patients were diagnosed with unresectable stage IIIA, IIIB, or IV or post-operative recurrent NSCLC at the Juntendo University Hospital. Seventeen patients were transferred to other hospitals immediately after diagnosis. A total of 515 patients attended our hospital and were enrolled in this case control study. We divided all patients into two groups, patients with and without CI. Then, we evaluated the differences between the two groups in any items.
Data regarding the patients’ baseline characteristics at the time of diagnosis of advanced NSCLC or post-operative recurrence were retrospectively collected, including age, sex, smoking history, Eastern Cooperative Oncology Group (ECOG)-PS, histological type, clinical stage, brain metastasis, and complications (hypertension, diabetes, hyperlipidemia, atrial fibrillation and old myocardial infarction).
CI was firstly detected by symptom and neurological examination and confirmed by brain magnetic resonance imaging (MRI) including diffusion-weighted MRI and neurologist. Blood examinations, especially d-dimer levels, were evaluated in patients with CI. For patients with CI, the clinical course before and after CI and survival time from the onset of CI were evaluated. Overall survival (OS) from diagnosis of advanced NSCLC or post-operative recurrence after radical surgery or chemoradio/radiotherapy was evaluated and compared between patients with CI and without CI.
All patients involved in this study provided verbal informed consent for the use of their medical data. This study protocol was approved by the Juntendo University Ethical Committee and registered under number 26–635.
Statistical method
We used the chi square test, Fisher's exact test, or Wilcoxon two-sample test to compare patient characteristics. Univariate and multivariate analyses were performed using logistic regression to assess the risk factors for CI. OS was plotted using the Kaplan–Meier method. Differences in OS were analyzed using the log-rank test, and hazard ratio (HR) was calculated by cox proportional hazard model. All p-values <0.05 were considered statistically significant. All statistical analyses were performed using SPSS ver. 15.0 for Windows (Chicago, IL, USA).
Discussion
In this study, we found that the incidence of CI was 2.9 % in advanced or post-operative recurrent NSCLC, and brain metastasis was the only risk factor for the development of CI in patients with advanced or post-operative recurrent NSCLC. In addition, the incidence of CI in patients with brain metastasis was significantly higher than that in patients without brain metastasis.
Few published studies have evaluated the association between CI and advanced NSCLC. Population-based data from Taiwan National Health Insurance revealed an increased risk of CI in lung cancer patients [
4]. In this report, the incidence of CI in all the stages of lung cancer was 21.80 per 1000 person-years. Conversely, the Dutch Pathology Registry linked to the PHARMO (Pharmaco Morbidity) medical record linkage system did not reveal increased risk of CI in lung cancer patients [
5]. In this report, the incidence of CI in all stages and histological types of lung cancer was 3.8 per 1000 person-years in 6 months after diagnosis with lung cancer. However, the incidence of CI in patients with advanced or post-operative recurrent NSCLC has not been reported yet. Two retrospective studies investigated the incidence of and risk factors for thromboembolic events including CI in lung cancer patients [
6,
7]. However, these reports included all stages and histological types of lung cancer and did not focus on CI. The current study is the first to evaluate the incidence of CI in advanced NSCLC, and the risk factors for CI in advanced NSCLC in terms of patient characteristics and complications.
An association between malignant neoplasms and thromboembolism, including arterial thromboembolic events and venous thromboembolism (VTE), has been reported by several groups. It has been reported that 13.2 % of newly diagnosed NSCLC patients have VTE [
8]. In that report, an increase in white blood cells was associated with VTE. Another group reported that incidence of VTE was higher among lung cancer patients with adenocarcinoma histology than among those with squamous cell carcinoma histology [
9]. Thromboembolism may be associated with poorly differentiated adenocarcinoma. Few case reports have described an association between poorly differentiated adenocarcinoma and thromboembolism in pancreatic, breast, and advanced ovarian cancers [
10‐
12]. In our study, 12 patients with CI had adenocarcinoma. However, there were no significant differences in histology between patients with CI and without CI. Further investigations with larger study populations are warranted to determine whether poorly differentiated adenocarcinoma is a risk factor for CI.
In general, CI was categorized as cardiac embolism, atherosclerosis, and lacunar infarction. On the other hand, it is difficult to easily classify etiology of CI in these patients. However, all of the patients with CI in our study had a sudden onset of severe neurological symptoms such as paralysis, dysarthria, and disturbance of consciousness. Therefore, lacunar infarction could not be an etiology of the CI in these patients. In our study, 10 patients had multiple infarctions and 5 patients had a single infarction on brain MRI. In patients with multiple infarctions, the CI must have been caused by thromboembolism. Seven patients had hypertension, and 1 patient had hyperlipidemia. In these patients, the occurrence of atherosclerosis might be related to the CI, although the development of thromboembolism/coagulation disorder is also related to CI. Some papers discuss the causes of CI in patients with cancer. One report described five causes of CI: direct tumor relation, coagulation disorders, infection, treatment related and paraneoplastic [
13]. In terms of coagulation disorders, cancer is known as one of the acquired prothrombotic states related to a high risk for stroke [
14]. Disseminated intravascular coagulation (DIC) is usually associated with advanced cancer. In this case, levels of specific markers for DIC, including
d-dimer, are often elevated. It has been reported that platinum compounds are associated with a higher risk for stroke including CI [
15]. Circulating endothelial-derived and platelet-derived microparticles occurring during the third or fourth infusion might contribute to cisplatin-induced stroke [
16]. Other anticancer agents, including cyclophosphamide, 5-fluorouracil, paclitaxel, and methotrexate, have been associated with the development of CI [
13,
17,
18]. Whereas 5 patients received chemotherapy with platinum agent (CDDP + PEM, CBDCA + PEM, and CBDCA + PTX), other patients were treated with PEM, DTX, EGFR-TKI or crizotinib at the onset of CI. Therefore, it is unclear that incidence of CI in patients treated with platinum agent is higher than in patients received non-platinum agent in this research. Most of the patients developed CI during first or second line chemotherapy. Because CI tends to occur immediately after diagnosis with advanced or post-operative recurrent NSCLC, attention should be paid if the patients have the risk of CI.
Ten patients had multiple micro infarctions, and 5 had single large infarctions on brain MRI. There was no evidence of direct relation of tumor on brain MRI. However, taking into account the fact that the incidence of CI in patients with brain metastasis was significantly higher than that in patients without brain metastasis, invasion or tumor emboli to vessels might cause CI. Moreover, cancer tissue releases the accelerator of coagulation and cause prothrombotic states. When the patients have brain metastases, accelerator of coagulation will increase locally and elevate the risk of CI. To our knowledge, there has been no report on the association between brain metastasis from any cancer and CI. However, it has been reported that the incidence ratio for subsequent ischemic stroke within 6 months after diagnosis in patients with cancer of the nervous system is the highest among all patients with any type of cancer [
19]. This report might support the findings of our study. There were no cardiogenic embolisms by physical examination and echocardiography, and the cause of CI in 10 patients with multiple and micro CIs could be categorized as coagulation disorders. CI developed during treatment in 14 out of 15 patients, and the cause of these CI could be categorized as treatment related. Of these patients, 12 developed CI during chemotherapy. Cytotoxic agents have been reported as risk factors for CI; however, 4 patients in our study experienced CI during treatment with molecular targeted agents.
Only one patient with CI was able to receive anticancer therapy after development of CI. Median survival time from onset of CI was 36 days. OS in patients with CI was significantly shorter than that in those without CI. These findings suggest that development of CI contributed to a worse prognosis in patients with advanced and recurrent NSCLC. Generally, the prognosis of advanced NSCLC patients is improving due to the development of chemotherapy, and control of adverse events and complications during chemotherapy, including CI, is becoming more important. The prophylaxis of CI in advanced NSCLC during treatment should be examined in future studies.
This analysis has several limitations. First, this was a retrospective study. However, although we might miss asymptomatic CI, the onset of CI is easy to detect, and therefore its frequency might not differ significantly from prospective evaluations. Moreover, asymptomatic CI is not significant in clinical practice. Secondly, this study did not include blood test findings in the analysis of risk factors for CI. However, although a study revealed an increased white blood cell count associated with VTE, blood test findings are not commonly known as risk factors for CI, and we assessed hyperlipidemia as a risk factor.
Competing interests
The authors declare that they have no competing interests.
Authors’ contributions
MK and TS conceived and designed the study. MK, TS and KeMo analyzed the data. RyKa, YH, YN, KeMu, RS, RyKo, NS and FT contributed to acquisition of clinical data. MK and TS wrote the manuscript. KT provided final approval of the version to be published. All authors read and approved the final manuscript.