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SiRNA & MiRNA.pptx

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SIRAJUDDIN MOLLA

SiRNA & MiRNA

Health & Medicine
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Seminar topic: siRNA and miRNA PRESENTED BY: SIRAJUDDIN MOLLA M.Phram, 1st Semester DEPARTMENT OF PHARMACOLOGY SPER, JAMIA HAMDARD 1
Index • RNA interference (RNAi) • siRNA (Small interfering RNA) • Function of siRNA • siRNA Production and Mechanism of action • miRNA (microRNA) • miRNA Production and Mechanism of action • Functions of miRNAs • Differences between miRNA and siRNA • miRNA and disease • miRNA and the nervous system • Importance of miRNA 2
• RNA interference (RNAi), the biological mechanism by which double stranded RNA (dsRNA) induces gene silencing by targeting complementary mRNA for degradation • Also called post transcriptional gene silencing (PTSG). • Play important role in post translational gene transposon regulation, defending cells against viruses. • 2 types of small silencing RNA molecules a) siRNA b) miRNA RNA interference (RNAi) 3
• Small interfering RNA (siRNA), sometimes known as short interfering RNA or silencing RNA. • It is a class of double-stranded, non-coding RNA molecules. • 20-25 base pairs in length • It is similar to miRNA • Operating within the RNA interference (RNAi) pathway by the enzyme Dicer. • It interferes with the expression of specific genes with complementary nucleotide sequences by degrading mRNA after transcription, resulting no translation. siRNA (Small interfering RNA) 4
 Small (or short) interfering RNA (siRNA) is the commonly used RNA interference (RNAi) tool for inducing short-term silencing of protein coding genes.  It is a double stranded RNA molecule which interferes with the expression of specific genes by degrading mRNA after transcription & preventing translation. Function of siRNA 5
• The first step of RNAi involves processing and cleavage of longer double-stranded RNA into siRNAs generally bearing a 2 nucleotide overhang on the 3' end of each strand. • The enzyme responsible for this processing is an RNase III-like enzyme termed Dicer. • Dicer domain includes an ATPase/RNA helicase domain, catalytic RNAase lll family enzyme. • Dicer and dsRNA binding protein  form RISC loading complex • RISC (RNA induced silencing complex). • After that load the RNA duplex into RISC. siRNA Production and Mechanism of action 6
Long dsRNA RISC-loading complex RISC recycling Guide-strand selection, passenger- strand cleavage/ejecti on Passenger- strand Guide- strand Dicer processing of long dsRNA Target mRNA slicin g 5’ 3’ 5’ 3’ Dicer siRNA 3’ TRBP (transactivation response element RNA-binding protein) 7
siRNA Production and Mechanism of action • The first step of RNAi involves processing and cleavage of longer double-stranded RNA into siRNAs generally bearing a 2 nucleotide overhang on the 3' end of each strand. • The enzyme responsible for this processing is an RNase III-like enzyme termed Dicer. • Dicer domain includes an ATPase/RNA helicase domain, catalytic RNAase lll family enzyme. • Dicer and dsRNA binding protein  form RISC loading complex • RISC (RNA induced silencing complex). • After that load the RNA duplex into RISC. 8
• Within the RISC complex, siRNA strands are separated and the strand with the more stable 5' end is typically integrated to the active RISC complex (guide RNA). • The antisense single-stranded siRNA component then guides and aligns the RIS complex on the target mRNA. • The action of catalytic RISC protein a member of the Argonaut family (Ago-2) having endonuclease activity  mRNA is cleaved which is complementary to their bound siRNA. stop translation When siRNA completely forms base pairing with target mRNA mRNA degrade otherwise inhibits mRNA to bind with ribosome Contd.. 9
miRNA (microRNA) A miRNA is small non-coding RNAs molecule Found only in eukaryotic cells (plants, animals) and sometimes in viruses. miRNAs are defined as 21-25 (avg. 22) nucleotide single-stranded RNAs (ssRNAs), which are produced from hairpin shaped precursors Transcribed by RNA polymerase II from independent genes or introns of protein-coding genes  miRNA functions in RNA silencing and post-transcriptional regulation of gene expression via base-pairing with complementary sequences within mRNA molecules. They play important gene-regulatory roles in both plants and animals. The first miRNA (lin-4) was discovered in C.elegans in the year 1993. 10
The pri-miRNA is processed within the nucleus to a precursor miRNA (pre-miRNA) by Drosha, a class 2 RNase III enzyme. The transport of pre-miRNAs to the cytoplasm is mediated by exportin-5 (EXP-5). In the cytoplasm, they are further processed to become mature miRNAs by Dicer, an RNase III type protein and loaded onto the Argonaute (ago) protein to produce the effector RNA-induced silencing complex (RISC). After that Followed the same pathway as siRNA miRNA Production and Mechanism of action 11
Chromosome having specific gene to produce miRNA Transcription RNA Pol II or III Primary or pri-miRNA Having complementary base pair itself forms hairpin structure (imperfect) Drosha (endonuclease) Pasha (droshophila) DGCR8 (mammals) Pre miRNA 70bp cytoplasm nucleu s Exportin 5 miRN A 12
The pri-miRNA is processed within the nucleus to a precursor miRNA (pre-miRNA) by Drosha (endonuclease), a class-2 Rnase-III family enzyme. Pasha (in Droshophila) and DGCR8 (in mammals) act as RNA binding protein The transport of pre-miRNAs to the cytoplasm is mediated by exportin-5 (EXP-5). In the cytoplasm, they are further processed to become mature miRNAs by Dicer, an RNase III type protein and loaded onto the Argonaute (ago) protein to produce the effector RNA-induced silencing complex (RISC). After that Followed the same pathway as siRNA miRNA Production and Mechanism of action 13
About 50% of the annotated human miRNAs map within fragile sites of chromosomes, which are areas of the genome that are associated with various human cancers. Recent evidence indicates that miRNAs can function as tumour suppressors and oncogenes, and they are therefore referred to 'oncomirs’. Gene therapies that use miRNAs might be an effective approach to blocking tumour progression. miR-15 and miR-16, which negatively regulate BCL2, are promising candidates for cancer treatment. Functions of miRNAs 14
Properties miRNA siRNA Origin found in Animals, plants, protists found in Ainmals, fungi, plants, protists Biogenesis (nature of precursor) Cleavage of Single-stranded RNA molecules that forms short hairpin (imperfect stem-loop secondary structure) Cleavage of long bimolecular RNA duplexes or single stranded RNA that forms long extended hairpins Nature of regulatory target Regulate different genes or Genes other than those from which they were transcribed Mediate the silencing of the same (or very similar) genes from which they were originated or transcribed Action Some trigger degradation of mRNA, others inhibit translation Some trigger degradation of mRNA, others inhibit transcription endonuclease Dicer/drosha dependent Dicer dependent Differences between miRNA and siRNA 15
 Just as miRNA is involved in the normal functioning of eukaryotic cell, so has dysregulation of miRNA been associated with disease.  miRNA and inherited diseases: • A mutation in the seed region of miR-96 causes hereditary progressive hearing loss. • A mutation in the seed region of miR-184 causes hereditary keratoconus with anterior polar cataract. • Deletion of the miR-17-92 cluster causes skeletal and growth defects. miRNA and disease The seed sequence of a miRNA is defined as the first 2–8 nucleotides starting at the 5′ end and counting toward the 3′ end 16
 miRNAs appear to regulate the nervous systems. Neural miRNAs are involved at various stages of synaptic development, including • dendritogenesis (involving miR-134) • synapse formation • synapse maturation (where miR-134 and 138 are thought to be involved). miRNA and the nervous system 17
miRNAs represent small RNA molecules encoded in the genomes of plants and animals. These highly conserved 22 nudeotides long RNA sequences regulate the expression of genes by binding to the 3'untranslated regions (3’UTR) of specific mRNAs. A growing body of evidence shows that miRNAs are one of the key players in cell differentiation and growth, mobility and apoptosis (programmed cell death). Importance of miRNA 18
• Discovered a little over two decades ago, small interfering RNAs (siRNAs) and microRNAs (miRNAs) are noncoding RNAs with important roles in gene regulation. • They have recently been investigated as novel classes of therapeutic agents for the treatment of a wide range of disorders including cancers and infections. • Clinical trials of siRNA and miRNA-based drugs have been initiated. • The therapeutic approaches of siRNAs and miRNAs are different as well as physicochemical properties, delivery, and clinical applications. Novel siRNA and miRNA 19
• Therapeutic approaches based on siRNA involve the introduction of a synthetic siRNA into the target cells to elicit RNA interference (RNAi), thereby inhibiting the expression of a specific messenger RNA (mRNA) to produce a gene silencing effect.9 • By contrast, miRNA-based therapeutics comprise two approaches: miRNA inhibition and miRNA replacement. • Inhibition approach resembles antisense therapy,10 with synthetic stranded RNAs acting as miRNA antagonists (also known as or anti-miRs) to inhibit the action of the endogenous miRNAs. • In the replacement approach, synthetic miRNAs (also known as miRNA mimics) are used to mimic the function of the endogenous miRNAs.11 • It thus leads to mRNA degradation/inhibition, and produces a gene silencing effect. Therapeutic approaches 20
siRNA and miRNA as therapeutic agents • The specific gene silencing effect of siRNAs makes them useful tools for target identification and validation in drug discovery and development.38,39 • Since miRNAs have multiple mRNA targets and the disruption of their functions contributes to the development of many diseases including cancers, neurodegenerative disorders and cardiovascular diseases, their clinical use as biomarkers and in diagnostics is rapidly developing.40 • Furthermore, both siRNAs and miRNAs have huge potential as therapeutic agents. They can overcome the major limitation of traditional small drug molecules, which can only target certain classes of proteins. 21
• Even for protein-based drugs including monoclonal antibodies that are highly specific, their targets are mainly limited to cell- surface receptors or circulating proteins. • By contrast, siRNAs and miRNAs can downregulate the expression of virtually all genes and their mRNA transcripts. • Since many diseases result from the expression of undesired or mutated genes, or from overexpression of certain normal genes, discovery of siRNA and miRNA opens up a whole new therapeutic approach for the treatment of diseases by targeting genes that are involved in the pathological process. Contd.. 22
Design of therapeutic siRNA • The first essential step for successful siRNA therapy is the design of a siRNA sequence that is potent and specific to the intended mRNA to minimize any off- target effect. • A conventional siRNA consists of 19–21 nucleotides with two nucleotide overhangs at the 3′ end, usually TT and UU, which are important for recognition by the RNAi machinery.41 • Increasing the length of the dsRNA may enhance its potency, as demonstrated by an in vitro study that dsRNAs with 27 nucleotides were up to 100 times more potent than the conventional siRNAs with 21 nucleotides.42 • On the other hand, dsRNAs longer than 30 nucleotides 20 The interferon (IFN) pathway plays a critical role in the human immune response. Following viral infection, the human body triggers a complex regulatory system of innate and adaptive immune responses designed to defend against the virus. 23
• Compared with siRNAs, miRNAs have a broader therapeutic application. • Since more than 60% of the human protein-coding genes contain at least one conserved miRNA-binding site, together with the of numerous non-conserved sites, the majority of protein-coding genes are under the control of miRNAs.29 • The goal of miRNA replacement therapy using synthetic miRNAs (or miRNA mimics) is to achieve the same biological functions as the endogenous miRNAs. • Therefore the synthetic miRNAs should possess the ability to be loaded to RISC and silence the target mRNAs through the natural miRNA signaling pathway. Design of therapeutic miRNA 24
• A single-stranded RNA molecule containing the sequence that is identical to the guide strand of the mature miRNA could be functioned as miRNA mimic. • However, the double stranded miRNA containing both guide guide and passenger strands was found to be 100 to 1,000 times more potent than the single stranded one.4,14 • The double stranded structure can facilitate the proper loading of the RNA molecule into the RISC, thereby enhancing the gene silencing effect. 25 Contd..
• Therefore, designing miRNA mimics with a duplex structure has become the direction of therapeutic development. • Synthetic miRNA precursors with longer sequences a few extra nucleotides to a full-length pri-miRNA) have also been proposed as therapeutic agents.78 • Since pri-miRNAs require processing in the nucleus, whereas pre-miRNA do not, different strategies are required for the delivery of different types of miRNA mimics to their cellular targets.79 26 Contd..
• The first clinical trial of siRNA therapeutics was initiated in 2004,175 merely 6 years after the discovery of RNAi. • The rapid progress of siRNA advancing into clinical trials is perhaps due to the experience gained during the development of antisense and other nucleic acid-based therapies. • To date, around 30 siRNA candidates have reached various stages of clinical trials for the treatment of different diseases. • In comparison, the clinical development of miRNA as therapeutics is lagging behind, with only two miRNA therapeutics, both of which are indicated for the treatment of cancers, being registered in clinical trial to date. siRNA AND miRNA therapeutics in clinical studies 27
• The first miRNA therapeutic trial began in 2013 with the second one starting in early 2015. • Although siRNAs share many similarities with miRNAs, the relatively slow progress of miRNA therapeutics could due to their uncertain mechanism of action and specificity. • The diverse potential applications of miRNAs (e.g., as drug target and biomarkers) may also have distracted from their development as therapeutic agents. 28 Contd..
Therapeutic indications of siRNA and miRNA therapeutics. 29
• Synthetic siRNAs and miRNAs hold great promises as new classes of therapeutic agents by silencing the gene(s) of interest. • They have been studied for the treatment of various human diseases including cancers, viral infections, ocular conditions, genetic disorders, and cardiovascular diseases. • The most attractive aspect of siRNA and miRNA therapeutics is their ability to target virtually any gene(s), which may not be possible with small molecules or protein-based drugs. • While the therapeutic efficacy of siRNAs and miRNAs has been successfully demonstrated in vivo, several technical barriers still need to be overcome in order for these RNA molecules to be used clinically. • The experience from antisense and gene therapy has contributed to the rapid progress of siRNAs and miRNAs into clinical Conclusions and future prospects 30
• Currently, the development of siRNAs is advancing ahead of miRNAs, with a larger number of candidates already entered clinical trials, possibly due to the uncertainties of the complex roles of miRNAs during the early years of their discovery. • With the recent surge in intensive research concerning miRNAs, it can be expected that significant advance will be made for their future role in therapeutics. 31 Contd..
1. The Cell, A Molecular Approach. Geoffrey M Cooper. 2. Pharmacogenomics: The Search for Individualized Therapies. Edited by J. Licinio and M -L. Wong 4. Molecular Pharmacology: From DNA to Drug Discovery. John Dickenson et.al 5. Basic Cell Culture protocols by Cheril D.Helgason and Cindy L.Miller 6. Basic Cell Culture (Practical Approach ) by J. M. Davis (Editor) 7. Animal Cell Culture: A Practical Approach by John R. Masters (Editor) https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4877448/#:~:text=Discovered%2 0a%20little%20over%20two,disorders%20including%20cancers%20and%20infect ions. References 32
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SiRNA & MiRNA.pptx

  • 1. Seminar topic: siRNA and miRNA PRESENTED BY: SIRAJUDDIN MOLLA M.Phram, 1st Semester DEPARTMENT OF PHARMACOLOGY SPER, JAMIA HAMDARD 1
  • 2. Index • RNA interference (RNAi) • siRNA (Small interfering RNA) • Function of siRNA • siRNA Production and Mechanism of action • miRNA (microRNA) • miRNA Production and Mechanism of action • Functions of miRNAs • Differences between miRNA and siRNA • miRNA and disease • miRNA and the nervous system • Importance of miRNA 2
  • 3. • RNA interference (RNAi), the biological mechanism by which double stranded RNA (dsRNA) induces gene silencing by targeting complementary mRNA for degradation • Also called post transcriptional gene silencing (PTSG). • Play important role in post translational gene transposon regulation, defending cells against viruses. • 2 types of small silencing RNA molecules a) siRNA b) miRNA RNA interference (RNAi) 3
  • 4. • Small interfering RNA (siRNA), sometimes known as short interfering RNA or silencing RNA. • It is a class of double-stranded, non-coding RNA molecules. • 20-25 base pairs in length • It is similar to miRNA • Operating within the RNA interference (RNAi) pathway by the enzyme Dicer. • It interferes with the expression of specific genes with complementary nucleotide sequences by degrading mRNA after transcription, resulting no translation. siRNA (Small interfering RNA) 4
  • 5.  Small (or short) interfering RNA (siRNA) is the commonly used RNA interference (RNAi) tool for inducing short-term silencing of protein coding genes.  It is a double stranded RNA molecule which interferes with the expression of specific genes by degrading mRNA after transcription & preventing translation. Function of siRNA 5
  • 6. • The first step of RNAi involves processing and cleavage of longer double-stranded RNA into siRNAs generally bearing a 2 nucleotide overhang on the 3' end of each strand. • The enzyme responsible for this processing is an RNase III-like enzyme termed Dicer. • Dicer domain includes an ATPase/RNA helicase domain, catalytic RNAase lll family enzyme. • Dicer and dsRNA binding protein  form RISC loading complex • RISC (RNA induced silencing complex). • After that load the RNA duplex into RISC. siRNA Production and Mechanism of action 6
  • 7. Long dsRNA RISC-loading complex RISC recycling Guide-strand selection, passenger- strand cleavage/ejecti on Passenger- strand Guide- strand Dicer processing of long dsRNA Target mRNA slicin g 5’ 3’ 5’ 3’ Dicer siRNA 3’ TRBP (transactivation response element RNA-binding protein) 7
  • 8. siRNA Production and Mechanism of action • The first step of RNAi involves processing and cleavage of longer double-stranded RNA into siRNAs generally bearing a 2 nucleotide overhang on the 3' end of each strand. • The enzyme responsible for this processing is an RNase III-like enzyme termed Dicer. • Dicer domain includes an ATPase/RNA helicase domain, catalytic RNAase lll family enzyme. • Dicer and dsRNA binding protein  form RISC loading complex • RISC (RNA induced silencing complex). • After that load the RNA duplex into RISC. 8
  • 9. • Within the RISC complex, siRNA strands are separated and the strand with the more stable 5' end is typically integrated to the active RISC complex (guide RNA). • The antisense single-stranded siRNA component then guides and aligns the RIS complex on the target mRNA. • The action of catalytic RISC protein a member of the Argonaut family (Ago-2) having endonuclease activity  mRNA is cleaved which is complementary to their bound siRNA. stop translation When siRNA completely forms base pairing with target mRNA mRNA degrade otherwise inhibits mRNA to bind with ribosome Contd.. 9
  • 10. miRNA (microRNA) A miRNA is small non-coding RNAs molecule Found only in eukaryotic cells (plants, animals) and sometimes in viruses. miRNAs are defined as 21-25 (avg. 22) nucleotide single-stranded RNAs (ssRNAs), which are produced from hairpin shaped precursors Transcribed by RNA polymerase II from independent genes or introns of protein-coding genes  miRNA functions in RNA silencing and post-transcriptional regulation of gene expression via base-pairing with complementary sequences within mRNA molecules. They play important gene-regulatory roles in both plants and animals. The first miRNA (lin-4) was discovered in C.elegans in the year 1993. 10
  • 11. The pri-miRNA is processed within the nucleus to a precursor miRNA (pre-miRNA) by Drosha, a class 2 RNase III enzyme. The transport of pre-miRNAs to the cytoplasm is mediated by exportin-5 (EXP-5). In the cytoplasm, they are further processed to become mature miRNAs by Dicer, an RNase III type protein and loaded onto the Argonaute (ago) protein to produce the effector RNA-induced silencing complex (RISC). After that Followed the same pathway as siRNA miRNA Production and Mechanism of action 11
  • 12. Chromosome having specific gene to produce miRNA Transcription RNA Pol II or III Primary or pri-miRNA Having complementary base pair itself forms hairpin structure (imperfect) Drosha (endonuclease) Pasha (droshophila) DGCR8 (mammals) Pre miRNA 70bp cytoplasm nucleu s Exportin 5 miRN A 12
  • 13. The pri-miRNA is processed within the nucleus to a precursor miRNA (pre-miRNA) by Drosha (endonuclease), a class-2 Rnase-III family enzyme. Pasha (in Droshophila) and DGCR8 (in mammals) act as RNA binding protein The transport of pre-miRNAs to the cytoplasm is mediated by exportin-5 (EXP-5). In the cytoplasm, they are further processed to become mature miRNAs by Dicer, an RNase III type protein and loaded onto the Argonaute (ago) protein to produce the effector RNA-induced silencing complex (RISC). After that Followed the same pathway as siRNA miRNA Production and Mechanism of action 13
  • 14. About 50% of the annotated human miRNAs map within fragile sites of chromosomes, which are areas of the genome that are associated with various human cancers. Recent evidence indicates that miRNAs can function as tumour suppressors and oncogenes, and they are therefore referred to 'oncomirs’. Gene therapies that use miRNAs might be an effective approach to blocking tumour progression. miR-15 and miR-16, which negatively regulate BCL2, are promising candidates for cancer treatment. Functions of miRNAs 14
  • 15. Properties miRNA siRNA Origin found in Animals, plants, protists found in Ainmals, fungi, plants, protists Biogenesis (nature of precursor) Cleavage of Single-stranded RNA molecules that forms short hairpin (imperfect stem-loop secondary structure) Cleavage of long bimolecular RNA duplexes or single stranded RNA that forms long extended hairpins Nature of regulatory target Regulate different genes or Genes other than those from which they were transcribed Mediate the silencing of the same (or very similar) genes from which they were originated or transcribed Action Some trigger degradation of mRNA, others inhibit translation Some trigger degradation of mRNA, others inhibit transcription endonuclease Dicer/drosha dependent Dicer dependent Differences between miRNA and siRNA 15
  • 16.  Just as miRNA is involved in the normal functioning of eukaryotic cell, so has dysregulation of miRNA been associated with disease.  miRNA and inherited diseases: • A mutation in the seed region of miR-96 causes hereditary progressive hearing loss. • A mutation in the seed region of miR-184 causes hereditary keratoconus with anterior polar cataract. • Deletion of the miR-17-92 cluster causes skeletal and growth defects. miRNA and disease The seed sequence of a miRNA is defined as the first 2–8 nucleotides starting at the 5′ end and counting toward the 3′ end 16
  • 17.  miRNAs appear to regulate the nervous systems. Neural miRNAs are involved at various stages of synaptic development, including • dendritogenesis (involving miR-134) • synapse formation • synapse maturation (where miR-134 and 138 are thought to be involved). miRNA and the nervous system 17
  • 18. miRNAs represent small RNA molecules encoded in the genomes of plants and animals. These highly conserved 22 nudeotides long RNA sequences regulate the expression of genes by binding to the 3'untranslated regions (3’UTR) of specific mRNAs. A growing body of evidence shows that miRNAs are one of the key players in cell differentiation and growth, mobility and apoptosis (programmed cell death). Importance of miRNA 18
  • 19. • Discovered a little over two decades ago, small interfering RNAs (siRNAs) and microRNAs (miRNAs) are noncoding RNAs with important roles in gene regulation. • They have recently been investigated as novel classes of therapeutic agents for the treatment of a wide range of disorders including cancers and infections. • Clinical trials of siRNA and miRNA-based drugs have been initiated. • The therapeutic approaches of siRNAs and miRNAs are different as well as physicochemical properties, delivery, and clinical applications. Novel siRNA and miRNA 19
  • 20. • Therapeutic approaches based on siRNA involve the introduction of a synthetic siRNA into the target cells to elicit RNA interference (RNAi), thereby inhibiting the expression of a specific messenger RNA (mRNA) to produce a gene silencing effect.9 • By contrast, miRNA-based therapeutics comprise two approaches: miRNA inhibition and miRNA replacement. • Inhibition approach resembles antisense therapy,10 with synthetic stranded RNAs acting as miRNA antagonists (also known as or anti-miRs) to inhibit the action of the endogenous miRNAs. • In the replacement approach, synthetic miRNAs (also known as miRNA mimics) are used to mimic the function of the endogenous miRNAs.11 • It thus leads to mRNA degradation/inhibition, and produces a gene silencing effect. Therapeutic approaches 20
  • 21. siRNA and miRNA as therapeutic agents • The specific gene silencing effect of siRNAs makes them useful tools for target identification and validation in drug discovery and development.38,39 • Since miRNAs have multiple mRNA targets and the disruption of their functions contributes to the development of many diseases including cancers, neurodegenerative disorders and cardiovascular diseases, their clinical use as biomarkers and in diagnostics is rapidly developing.40 • Furthermore, both siRNAs and miRNAs have huge potential as therapeutic agents. They can overcome the major limitation of traditional small drug molecules, which can only target certain classes of proteins. 21
  • 22. • Even for protein-based drugs including monoclonal antibodies that are highly specific, their targets are mainly limited to cell- surface receptors or circulating proteins. • By contrast, siRNAs and miRNAs can downregulate the expression of virtually all genes and their mRNA transcripts. • Since many diseases result from the expression of undesired or mutated genes, or from overexpression of certain normal genes, discovery of siRNA and miRNA opens up a whole new therapeutic approach for the treatment of diseases by targeting genes that are involved in the pathological process. Contd.. 22
  • 23. Design of therapeutic siRNA • The first essential step for successful siRNA therapy is the design of a siRNA sequence that is potent and specific to the intended mRNA to minimize any off- target effect. • A conventional siRNA consists of 19–21 nucleotides with two nucleotide overhangs at the 3′ end, usually TT and UU, which are important for recognition by the RNAi machinery.41 • Increasing the length of the dsRNA may enhance its potency, as demonstrated by an in vitro study that dsRNAs with 27 nucleotides were up to 100 times more potent than the conventional siRNAs with 21 nucleotides.42 • On the other hand, dsRNAs longer than 30 nucleotides 20 The interferon (IFN) pathway plays a critical role in the human immune response. Following viral infection, the human body triggers a complex regulatory system of innate and adaptive immune responses designed to defend against the virus. 23
  • 24. • Compared with siRNAs, miRNAs have a broader therapeutic application. • Since more than 60% of the human protein-coding genes contain at least one conserved miRNA-binding site, together with the of numerous non-conserved sites, the majority of protein-coding genes are under the control of miRNAs.29 • The goal of miRNA replacement therapy using synthetic miRNAs (or miRNA mimics) is to achieve the same biological functions as the endogenous miRNAs. • Therefore the synthetic miRNAs should possess the ability to be loaded to RISC and silence the target mRNAs through the natural miRNA signaling pathway. Design of therapeutic miRNA 24
  • 25. • A single-stranded RNA molecule containing the sequence that is identical to the guide strand of the mature miRNA could be functioned as miRNA mimic. • However, the double stranded miRNA containing both guide guide and passenger strands was found to be 100 to 1,000 times more potent than the single stranded one.4,14 • The double stranded structure can facilitate the proper loading of the RNA molecule into the RISC, thereby enhancing the gene silencing effect. 25 Contd..
  • 26. • Therefore, designing miRNA mimics with a duplex structure has become the direction of therapeutic development. • Synthetic miRNA precursors with longer sequences a few extra nucleotides to a full-length pri-miRNA) have also been proposed as therapeutic agents.78 • Since pri-miRNAs require processing in the nucleus, whereas pre-miRNA do not, different strategies are required for the delivery of different types of miRNA mimics to their cellular targets.79 26 Contd..
  • 27. • The first clinical trial of siRNA therapeutics was initiated in 2004,175 merely 6 years after the discovery of RNAi. • The rapid progress of siRNA advancing into clinical trials is perhaps due to the experience gained during the development of antisense and other nucleic acid-based therapies. • To date, around 30 siRNA candidates have reached various stages of clinical trials for the treatment of different diseases. • In comparison, the clinical development of miRNA as therapeutics is lagging behind, with only two miRNA therapeutics, both of which are indicated for the treatment of cancers, being registered in clinical trial to date. siRNA AND miRNA therapeutics in clinical studies 27
  • 28. • The first miRNA therapeutic trial began in 2013 with the second one starting in early 2015. • Although siRNAs share many similarities with miRNAs, the relatively slow progress of miRNA therapeutics could due to their uncertain mechanism of action and specificity. • The diverse potential applications of miRNAs (e.g., as drug target and biomarkers) may also have distracted from their development as therapeutic agents. 28 Contd..
  • 29. Therapeutic indications of siRNA and miRNA therapeutics. 29
  • 30. • Synthetic siRNAs and miRNAs hold great promises as new classes of therapeutic agents by silencing the gene(s) of interest. • They have been studied for the treatment of various human diseases including cancers, viral infections, ocular conditions, genetic disorders, and cardiovascular diseases. • The most attractive aspect of siRNA and miRNA therapeutics is their ability to target virtually any gene(s), which may not be possible with small molecules or protein-based drugs. • While the therapeutic efficacy of siRNAs and miRNAs has been successfully demonstrated in vivo, several technical barriers still need to be overcome in order for these RNA molecules to be used clinically. • The experience from antisense and gene therapy has contributed to the rapid progress of siRNAs and miRNAs into clinical Conclusions and future prospects 30
  • 31. • Currently, the development of siRNAs is advancing ahead of miRNAs, with a larger number of candidates already entered clinical trials, possibly due to the uncertainties of the complex roles of miRNAs during the early years of their discovery. • With the recent surge in intensive research concerning miRNAs, it can be expected that significant advance will be made for their future role in therapeutics. 31 Contd..
  • 32. 1. The Cell, A Molecular Approach. Geoffrey M Cooper. 2. Pharmacogenomics: The Search for Individualized Therapies. Edited by J. Licinio and M -L. Wong 4. Molecular Pharmacology: From DNA to Drug Discovery. John Dickenson et.al 5. Basic Cell Culture protocols by Cheril D.Helgason and Cindy L.Miller 6. Basic Cell Culture (Practical Approach ) by J. M. Davis (Editor) 7. Animal Cell Culture: A Practical Approach by John R. Masters (Editor) https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4877448/#:~:text=Discovered%2 0a%20little%20over%20two,disorders%20including%20cancers%20and%20infect ions. References 32
  • 33. 33