Breast cancer is the most frequentl

Breast cancer is the most frequently diagnosed malignancy and is the leading cause of cancer
death among females. It accounts for 23% of all cancer cases and 14% of cancer deaths worldwide
[1]. Approximately 232,670 women in the United States are estimated to be diagnosed with invasive
breast cancer in 2014, and 40,000 women will die from it [2]. At present, mortality rates are
declining in several Western countries because of the increased implementation ofmammographic
screening and adjuvant systemic therapies for newly diagnosed cases. However, the longterm
survival rate and prognosis of advanced-stage patients remain poor, especially in developing
countries [2,3]. Currently, both tissue- and serum-based tumor biomarkers are widely used to
screen early-stage breast cancer and to predict either its progression or recurrence in advance.
These biomarkers include human epidermal growth factor 2 receptor (Her2), estrogen receptor
(ER), progesterone receptor (PR), and p53 [4]. Breast cancer is quite complex and heterogeneous
in its development, progress, and response to treatment; therefore, researchers are encouraged to
identify novel biomarkers for the optimization of breast cancer management.
MiRNAs are a class of 18–25 nucleotide, non-coding RNAs that are significant in the regulation
of post-transcriptional gene expression [5]. Studies have shown that miRNAs are involved
in virtually all biological processes, including cell proliferation, differentiation, and apoptosis
[5,6].Moreover, miRNAs act as critical regulators of tumorigenesis and are believed to be involved
in tumor development and progression [7]. Calin et al. were the first to provide direct
evidence of regarding the function of miRNA in human cancer. They reported that aberrant expressions
of both miR-15 and miR-16 are related to chronic lymphocytic leukemia [8]. Many
subsequent studies identified several miRNAs that are correlated with various human cancers
[9,10]. In addition, clinical and quantitative studies determined that the expression levels of
some miRNAs are associated with either the stages of diseases or with cancer survival outcomes
[11,12]; thus, miRNAs may serve as potential diagnostic or prognostic biomarkers of cancer.
MiR-21 acts as an oncogene and is among the most frequently observed cancer-related miRNAs.
It is consistently dysregulated in many types of cancer [13] and is a key factor in tumorigenesis
and tumor suppression because it targets tumor suppressor genes such as tropomyosin
1, programmed cell death 4, and phosphatase and tensin homolog [14–17]. Recent accumulated
evidence supports the concept of miR-21 as a potential diagnostic or prognostic biomarker
in various types of cancer, such as colon cancer, pancreatic cancer, and lung cancer [18–20].
Nonetheless, some of these studies fail to confirm the association between miR-21 and cancer
survival outcomes [21,22]; as a result, their results remain controversial. Moreover, the prognostic
value of miR-21 varies in different clinical studies with respect to breast cancer [23,24].
Therefore, we conduct this meta-analysis to determine whether miR-21 can predict poor survival
rates in breast cancer patients.