Introduction

The discovery of lin-4 in Caenorhabditis elegans,1, 2, 3, 4, 5 the first microRNA (miRNA), led to the identification of several hundred other miRNA molecules. MiRNAs are short noncoding RNA molecules of roughly 19–24 nucleotides in length and are a large class, with more than 1,000 members, of small-regulatory RNAs in mammalian genomes. MiRNAs are initially processed as a primary miRNA (pri-miRNA) transcript by RNA polymerase II (or by RNA polymerase III in rare cases) and associated transcription factors. The pri-miRNAs are further processed by Drosha, a nuclear RNase III enzyme, to produce precursor miRNAs (pre-miRNAs). The pre-miRNAs are then transported out of the nucleus into the cytoplasm where they are further processed by the Dicer, another RNase III-familial endonuclease, to become ∼22 base-pairing (bp) miRNA duplexes. Mature miRNAs are then unwound from miRNA duplexes and loaded into the RNA-induced silencing complex (RISC). The RISC with the mature miRNAs can regulate gene expression by binding to the mRNA transcripts of target genes, usually at the 3′ untranslated regions (3′-UTRs). Cancer Biology and MicroRNAs – Essay Example. The miRNA-RISC complex can block translation of target mRNA into protein and/or induce degradation of target mRNA transcript (see Fig. 1).6, 7, 8

Binding of an animal miRNA to its target gene transcript relies mainly on a 6–8 nucleotide pair region of near perfect complementarity between the 5′ end (i.e., the ‘seed region’) of the miRNA and its target mRNA sequence. Although miRNAs usually bind to the 3′ UTRs of target transcripts, evidence is emerging that the target sites can be located outside of the 3′ UTRs, such as 5′ untranslated regions (5′-UTRs) or protein-coding regions. Interestingly, recent studies have demonstrated that allelic and sequence variants can i) create a new miRNA binding site where one did not exist before, ii) remove a miRNA binding site, or iii) change the affinity of a particular miRNA for a binding site.9, 10 Furthermore, as a single miRNA can regulate tens or even hundreds of different target genes while a single gene may be regulated by multiple miRNAs; the miRNA-target networks are pretty complex.

This review will focus on the functions of miRNAs in the pathogenesis of tumors and the potential clinical implications of miRNAs in the diagnosis, prognosis and therapy of cancers. First, it will outline the functions of miRNAs in cancer biology as tumor suppressors and/or oncogenes and how miRNAs can synergistically work together. Next, it will discuss miRNAs related to cancer therapy/treatment. Finally, it will focus on miRNAs as diagnostic and prognostic tools in the context of the tumor itself and circulating in blood plasma. Cancer Biology and MicroRNAs – Essay Example.

The regulations and functions of MiRNAs in cancers

For the past ten years the study of miRNAs in eukaryotic organisms has grown exponentially and it has been well established that these small RNAs are master regulators of gene expression and multiple other biological processes. MiRNAs were first identified in the mid-1990s with the discovery of Let-7 and Lin-4 in a worm (Caenorhabditis elegans),1, 2, 11 but it was not until 2000/2001 when it was determined that these miRNAs exist and are highly conserved in multiple eukaryotic organisms and mammalian species.3, 4, 5 This was a major finding in the field of miRNAs, showing not only that they exist in multiple organisms but also they are likely major regulators of biological processes in these organisms. The next landmark event came soon after in 2002 and 2003 when it was found that miRNAs were aberrantly expressed in cancer12, 13, 14 and subsequently several seminal studies were reported in 2005 that provided compelling evidence to demonstrate the importance of miRNAs in cancer.15, 16, 17Since then, the study of miRNAs in cancer exploded dramatically and still represents a very important and challenging area of research (see examples in Table 1, Table 2).

Furthermore, it is becoming evident that an emerging hallmark of cancer is the dysregulation of miRNAs, both in the tumor itself and in the surrounding microenvironment. Future work in this field will undoubtedly ensure its position in the new hallmarks of cancer.18 Dysregulated miRNAs can contribute to tumorigenesis by playing tumor-suppressive and/or oncogenic roles. As exampled in Table 1, many miRNAs, including miR-29b,19, 20 miR-34b/c,21, 22 miR-126,23, 24, 25, 26, 27 miR-150,28 miR-155,29, 30 miR-181a/b,31, 32 miR-375,33 miR-494,34 miR-49535, 36 and miR-551a,35 play critical tumor-suppressor roles in tumorigenesis and/or mark a good prognosis for patients. These miRNAs have shown to have potent antitumorigenic properties. However, there are also numerous oncogenic miRNAs including miR-9,37miR-17-92,38, 39, 40 miR-21,41 miR-27a,42 miR-30a/c,43, miR-126,44 miR-181a/b,45, 46, 47 miR-196a,48 miR-196b,49 and miR-421.50 The intricate role of miRNAs in tumorigenesis appears to be simple yet it remains complicated. This can be attributed to several reasons briefly reviewed in the following section.

MiRNAs mediate drug response and themselves are modulated in therapy

As miRNAs were being linked to several hallmarks of cancer in tumor cells, there was a hypothesis that miRNA expression could be altered by cancer therapy and associated with drug response. This hypothesis is supported by two lines of evidence that are not mutually exclusive: differential expression of miRNAs in tumor cells before treatment has been associated with response to chemotherapy; changes in miRNA expression have been observed in cancer cells following treatment with effective therapy. It is highly likely that these observations are linked together within a single cancer (see Fig. 2). Cancer Biology and MicroRNAs – Essay Example. For example, it was found within lung cancer a group of miRNAs were regulated by epithelial growth factor receptor (EGFR) and hepatocyte growth factor receptor (MET).94 Both EGFR and MET are overexpressed in lung cancer driving tumorigenesis and, interestingly, the investigators found that these miRNAs bestowed resistance to tyrosine kinase therapy.94 Specifically, they found that gefitinib (a tyrosine kinase inhibitor) treatment inhibited miR-221, miR-222, miR-30b and miR-30c, all positively regulated by EGFR and MET, and resulted in increased apoptosis in lung cancer cell lines.94 Furthermore, increased expression of miR-30c, miR-221 and miR-222 in gefitinib-responsive cells attenuated sensitivity and knockdown of these miRNAs bestowed sensitivity to gefitinib in normally gefitinib-insensitive cells.94

Meanwhile, the effect of metabolism or chemotherapy-based diet on miRNA expression and subsequent tumorigenesis has also bee investigated. For example, Mandal et al found that the bioactive component of fish oil, docosahexaenoic acid (DHA), inhibited miR-21, a protumorigenic miRNA.41 Another group found the diet/microbe-derived short chain fatty acid butyrate, a known histone deacetylase (HDAC) inhibitor used in cancer treatment particularly in colon cancer, blocked tumorigenesis through inhibiting miR-106b expression and subsequently promoting expression of p21, a direct target of miR-106b.95 Similarly, it was reported that butyrate resulted in decreased expression of the oncogenic miRNA cluster miR-17-92; they found this similar result was observed in other HDAC inhibitors such as trichostatin A (TSA) and suberoylanilide hydroxamic acid (SAHA).96 Several of these inhibitors are clinically approved for the treatment of a few cancers and are currently being evaluated for other cancers, which provide a novel avenue for research.

Together these results show that miRNAs both modulate response to chemotherapy and are themselves modulated by chemotherapy. These effects can be direct or through indirect as are the examples of diet-induced miRNA changes. The new wave of cancer therapy is focusing on drugs that specifically target miRNAs as well as complementary signaling pathways to synergize with the routine use of chemotherapy in cancer patients.

MiRNA-based cancer therapy

Due to the central role of miRNAs in cancer initiation and progression, they have been a source of interest for several years, specifically whether these miRNAs can be targeted or not.97 As already described, it has been observed that several drugs can alter miRNA expression. Cancer Biology and MicroRNAs – Essay Example. Moreover, if certain cancers are particularly “addicted” to particular miRNAs (named oncomiR addiction) then targeting specific miRNAs selectively should minimize off-target toxicity.98 Investigators are interested in designing inhibitors for oncogenic miRNAs and mimics for tumor-suppressor miRNAs that can act alone or synergistically with currently approved treatments (see Fig. 2).99

In the past ten years several methods of design of miRNA inhibitors have been designed. One method of miRNA inhibition has been the use of modified nucleic acids that can bind and inhibit the mature miRNAs.99 An example of this is the anti-miR which can have various chemical modifications that enhance function and increase stability such as locked nucleic acids (LNAs),99, 100, 101 peptic nucleic acids, phosphorothioate modifications, 2′O-Me and 2′-fluoro substitutions and morpholinos.59, 99, 100, 101, 102, 103, 104, 105 Such miRNA inhibitors have been tested successfully in multiple experiments and are currently being evaluated for clinical purposes.101, 105 In contrast, nude miRNA mimics can be packaged directly with delivery vehicles for therapy.106

Another active area with miRNA research has been the delivery of miRNA inhibitors or miRNA mimics to target host regions. One effective method is the use of engineered viruses that induce miRNA inhibition through the expression of transcripts complementary to mature miRNA sequences. These viral delivery methods have had significant success in laboratory studies but have limited effectiveness in patients due to concerns about off-target effects of the viruses such as immunogenicity and chromosomal incorporations.107 Another limitation is the inability to specifically target the virus to the tumor and thereby generating toxicity as several of these miRNAs control host processes important for issues outside of the tumor.107, 108, 109 Another mechanism for the delivery of miRNA-based therapies is the use of nanoparticles.110, 111 The nanoparticle delivery method appears attractive because it avoids several of the concerns used for viral delivery systems.107 The nanoparticle delivery method has been shown to hold great potential.Cancer Biology and MicroRNAs – Essay Example.  For example, Su et al found that lipid nanoparticles that contained 2′fluoro-modified anti-miR-122 significantly inhibited tumor growth.110Another method recently developed was the use of biodegradable polymer nanoparticles containing anti-miRNAs to inhibit miR-155 in a mouse model of pre-B-cell lymphoma.111 Nanoparticles conjugated with targeting molecules for specific binding have also been designed and tested. For example, Huang et al designed transferring-conjugated anionic lipopolyplex nanoparticles carrying miR-29b and showed their specific binding to AML cells and significant anti-leukemia activities in vitro and in vivo.106

MiRNAs as biomarkers for diagnosis and prognosis in cancers

Currently, there are dozens of clinical trials that are assessing the correlation between miRNA expression and cancer diagnosis and prognosis. Several of these trials have been started in the past five years (www.clinicaltrials.gov) while new ones are being designed. Due to the pleiotropic effects of miRNAs they have been an attractive avenue for patient diagnosis evaluation and prognosis. Also, miRNAs, attributed to their size, are highly stable and resistant to RNAses and thus have a higher level of stability than mRNA. Cancer Biology and MicroRNAs – Essay Example.

New function of MiRNAs other than targeting mRNAs

Increasing evidence shows that both normal and tumor cells (especially circulating tumor cells (CTCs)162, 163 in terms of solid tumors) can package miRNAs in exosomes (10–100 nm in diameter), microvesicles (100–1000 nm), membrane microparticles (50–80 nm) and apoptotic bodies (50–500 nm) which appear to be specifically-packaged miRNAs.164 These miRNAs can control functions in both closely neighboring cells and distantly located cells. This provides a solid basis to study miRNAs in CTCs and in extracellular vesicles. Further, with new research it has been discovered that miRNAs can bind to proteins, challenging the current dogma of miRNAs acting solely on target mRNAs.165 Thus, miRNAs packed in these extracellular vesicles can have diverse effects outside of mRNA binding. This thought was very recently supported when it was discovered that miRNAs (miR-21 and miR-29a) within exosomes can bind to toll-like receptors (TLRs) and could activate immune cells as ligands for these receptors.165Although this might have been hypothesized with previous knowledge that single viral RNAs can be ligands for these receptors,166, 167 these findings have never been shown before in miRNAs and open up an entirely undiscovered and novel field looking at the function of miRNAs as ligands. Cancer Biology and MicroRNAs – Essay Example. Additionally, this could mean that miRNAs could be potential ligands for the large class of orphan receptors where no ligand has been identified to date168, 169 or they could be ligands for a myriad of other receptors.

Conclusions

As we look at the last decade of miRNA research in cancer biology and the incredible work that has been accomplished, it is clear that there is still much to be discovered. The future work in the next ten years will be focused on understanding how miRNAs regulate target genes in cancer initiation, progression, metastasis, relapse, and drug response and resistance, which will provide a more comprehensive mechanistic analysis of these noncoding RNAs. Furthermore, more noncoding RNAs are constantly being studied and are also an increasing area of focus. Future work will undoubtedly focus on the co-interaction and regulation of noncoding RNAs and how they together contribute to disease. Once we have gained this understanding, it will allow researchers to design better miRNA inhibitors or miRNA mimics that will guide the creation of new and more effective drug therapies. However, there are still lots of challenges to be solved before we applied miRNA-based therapies into the clinic to treat cancer patients.  Cancer Biology and MicroRNAs – Essay Example.