Your search keyword '"Snigdha Tiash"' showing total 26 results

1. Thieno[3,2-b]pyrrole 5-carboxamides as potent and selective inhibitors of Giardia duodenalis

Author

Christopher JS. Hart, Andrew G. Riches, Snigdha Tiash, Rebecca Abraham, Keely Fayd’Herbe, Ellis Joch, Bilal Zulfiqar, Melissa L. Sykes, Vicky M. Avery, Jan Šlapeta, Sam Abraham, John H. Ryan, and Tina S. Skinner-Adams

Subjects

Giardia duodenalis, Drug discovery, Thieno[3,2-b]pyrrole 5-carboxamides, Infectious and parasitic diseases, RC109-216

Abstract

Giardia duodenalis is the causative agent of the neglected diarrhoeal disease giardiasis. While often self-limiting, giardiasis is ubiquitous and impacts hundreds of millions of people annually. It is also a common gastro-intestinal disease of domestic pets, wildlife, and livestock animals. However, despite this impact, there is no vaccine for Giardia currently available. In addition, treatment relies on chemotherapies that are associated with increasing failure rates. To identify new treatment options for giardiasis we recently screened the Compounds Australia Scaffold Library for new chemotypes with selective anti-Giardia activity, identifying three compounds with sub-μM activity and promising selectivity. Here we extended these studies by examining the anti-Giardia activity of series CL9569 compounds. This compound series was of interest given the promising activity (IC50 1.2 μM) and selectivity demonstrated by representative compound, SN00798525 (1). Data from this work has identified an additional three thieno [3,2-b]pyrrole 5-carboxamides with anti-Giardia activity, including 2 which displayed potent cytocidal (IC50 ≤ 10 nM) and selective activity against multiple Giardia strains, including representatives from both human-infecting assemblages and metronidazole resistant parasites. Preclinical studies in mice also demonstrated that 2 is well-tolerated, does not impact the normal gut microbiota and can reduce Giardia parasite burden in these animals.

Published

2023

2. Plasmodium falciparum formins are essential for invasion and sexual stage development

Author

Sophie Collier, Emma Pietsch, Madeline Dans, Dawson Ling, Tatyana A. Tavella, Sash Lopaticki, Danushka S. Marapana, Mohini A. Shibu, Dean Andrew, Snigdha Tiash, Paul J. McMillan, Paul Gilson, Leann Tilley, and Matthew W. A. Dixon

Subjects

Biology (General), QH301-705.5

Abstract

Abstract The malaria parasite uses actin-based mechanisms throughout its lifecycle to control a range of biological processes including intracellular trafficking, gene regulation, parasite motility and invasion. In this work we assign functions to the Plasmodium falciparum formins 1 and 2 (FRM1 and FRM2) proteins in asexual and sexual blood stage development. We show that FRM1 is essential for merozoite invasion and FRM2 is required for efficient cell division. We also observed divergent functions for FRM1 and FRM2 in gametocyte development. Conditional deletion of FRM1 leads to a delay in gametocyte stage progression. We show that FRM2 controls the actin and microtubule cytoskeletons in developing gametocytes, with premature removal of the protein resulting in a loss of transmissible stage V gametocytes. Lastly, we show that targeting formin proteins with the small molecule inhibitor of formin homology domain 2 (SMIFH2) leads to a multistage block in asexual and sexual stage parasite development.

Published

2023

3. Deletion of the Plasmodium falciparum exported protein PTP7 leads to Maurer's clefts vesiculation, host cell remodeling defects, and loss of surface presentation of EMP1.

Author

Olivia M S Carmo, Gerald J Shami, Dezerae Cox, Boyin Liu, Adam J Blanch, Snigdha Tiash, Leann Tilley, and Matthew W A Dixon

Subjects

Immunologic diseases. Allergy, RC581-607, Biology (General), QH301-705.5

Abstract

Presentation of the variant antigen, Plasmodium falciparum erythrocyte membrane protein 1 (EMP1), at knob-like protrusions on the surface of infected red blood cells, underpins the parasite's pathogenicity. Here we describe a protein PF3D7_0301700 (PTP7), that functions at the nexus between the intermediate trafficking organelle, the Maurer's cleft, and the infected red blood cell surface. Genetic disruption of PTP7 leads to accumulation of vesicles at the Maurer's clefts, grossly aberrant knob morphology, and failure to deliver EMP1 to the red blood cell surface. We show that an expanded low complexity sequence in the C-terminal region of PTP7, identified only in the Laverania clade of Plasmodium, is critical for efficient virulence protein trafficking.

Published

2022

4. An image-based Pathogen Box screen identifies new compounds with anti-Giardia activity and highlights the importance of assay choice in phenotypic drug discovery

Author

Snigdha Tiash, Jake Saunders, Christopher J.S. Hart, John H. Ryan, Andrew G. Riches, and Tina S. Skinner-Adams

Subjects

Infectious and parasitic diseases, RC109-216

Abstract

Giardia duodenalis, the most prevalent human intestinal parasite causes the disease, giardiasis. On an annual basis G. duodenalis infects ~1 billion people, of which ~280 million develop symptomatic disease. Giardiasis can be severe and chronic, causing malnutrition, stunted growth and poor cognitive development in children. Current treatment options rely on drugs with declining efficacy and side-effects. To improve the health and well-being of millions of people world-wide, new anti-Giardia drugs with different modes of action to currently used drugs are required. The Medicines for Malaria Venture's Pathogen Box, a collection of bio-active compounds specifically chosen to stimulate infectious disease drug discovery, represents an opportunity for the discovery of new anti-Giardia agents. While the anti-Giardia activity of Pathogen Box compounds has been reported, this work failed to identify known anti-Giardia controls within the compound set. It also reported the activity of compounds previously screened and shown to be inactive by others, suggesting data may be inaccurate. Given these concerns the anti-Giardia activity of Pathogen Box compounds was re-assessed in the current study. Data from this work identified thirteen compounds with anti-Giardia IC50 values ≤2 μM. Five of these compounds were reference compounds (marketed drugs with known anti-microbial activity), or analogues of compounds with previously described anti-Giardia activity. However, eight, including MMV676358 and MMV028694, which demonstrated potent sub-μM IC50s against assemblage A, B and metronidazole resistant parasites (0.3 μM and 0.9 μM respectively), may represent new leads for future drug development. Interestingly, only four of these compounds were identified in the previously reported Pathogen Box screen highlighting the importance of assay selection and design when assessing compounds for activity against infectious agents. Keywords: Pathogen box, Giardia duodenalis, Drug discovery

Published

2020

5. A Subset Screen of the Compounds Australia Scaffold Library Identifies 7-Acylaminodibenzoxazepinones as Potent and Selective Hits for Anti-Giardia Drug Discovery

Author

Christopher J. S. Hart, Andrew G. Riches, Snigdha Tiash, Erin Clapper, Soumya Ramu, Johannes Zuegg, John H. Ryan, and Tina S. Skinner-Adams

Subjects

Giardia duodenalis, giardiasis, drug discovery, Compounds Australia Scaffold Library, acylaminodibenzoxazepinones, Biology (General), QH301-705.5

Abstract

On an annual basis the flagellate protozoan, Giardia duodenalis, is responsible for an estimated one billion human infections of which approximately two hundred million cause disease. However, the treatment of Giardia infections is reliant on a small group of chemotherapeutic classes that have a broad spectrum of antimicrobial activity and increasing treatment failure rates. To improve this situation, we need new drugs. In this study we screened the Compounds Australia Scaffolds Library for compounds with potent and selective activity against these parasites. Unlike previous drug discovery efforts that have focused on drug repurposing, this library is comprised of commercially available synthetic compounds arranged into lead-like scaffolds to facilitate structure activity relationship assessments and de novo drug discovery. A screen of 2451 compounds in this library identified 40 hits (>50% inhibitory activity at 10 µM, over 48 h). Secondary testing identified three compounds with IC50 values 50-fold selectivity for parasites over mammalian cells and a hit series, CL9406, comprising compounds with potent (lowest IC50 180 nM) and selective activity for Giardia parasites. The most promising compound in this series, SN00797640, displayed selective activity against assemblage A, B, and metronidazole resistant parasites which was parasiticidal (minimum lethal concentration 625 nM) and synergistic with albendazole. SN00797640 was well-tolerated when administered to mice at doses of 50 mg/kg daily for three days paving the way for pre-clinical in vivo activity assessment.

Published

2022

6. Role of Plasmodium falciparum Protein GEXP07 in Maurer’s Cleft Morphology, Knob Architecture, and P. falciparum EMP1 Trafficking

Author

Emma McHugh, Olivia M. S. Carmo, Adam Blanch, Oliver Looker, Boyin Liu, Snigdha Tiash, Dean Andrew, Steven Batinovic, Andy J. Y. Low, Hyun-Jung Cho, Paul McMillan, Leann Tilley, and Matthew W. A. Dixon

Subjects

malaria, protein trafficking, virulence determinants, Microbiology, QR1-502

Abstract

ABSTRACT The malaria parasite Plasmodium falciparum traffics the virulence protein P. falciparum erythrocyte membrane protein 1 (PfEMP1) to the surface of infected red blood cells (RBCs) via membranous organelles, known as the Maurer’s clefts. We developed a method for efficient enrichment of Maurer’s clefts and profiled the protein composition of this trafficking organelle. We identified 13 previously uncharacterized or poorly characterized Maurer’s cleft proteins. We generated transfectants expressing green fluorescent protein (GFP) fusions of 7 proteins and confirmed their Maurer’s cleft location. Using co-immunoprecipitation and mass spectrometry, we generated an interaction map of proteins at the Maurer’s clefts. We identified two key clusters that may function in the loading and unloading of PfEMP1 into and out of the Maurer’s clefts. We focus on a putative PfEMP1 loading complex that includes the protein GEXP07/CX3CL1-binding protein 2 (CBP2). Disruption of GEXP07 causes Maurer’s cleft fragmentation, aberrant knobs, ablation of PfEMP1 surface expression, and loss of the PfEMP1-mediated adhesion. ΔGEXP07 parasites have a growth advantage compared to wild-type parasites, and the infected RBCs are more deformable and more osmotically fragile. IMPORTANCE The trafficking of the virulence antigen PfEMP1 and its presentation at the knob structures at the surface of parasite-infected RBCs are central to severe adhesion-related pathologies such as cerebral and placental malaria. This work adds to our understanding of how PfEMP1 is trafficked to the RBC membrane by defining the protein-protein interaction networks that function at the Maurer’s clefts controlling PfEMP1 loading and unloading. We characterize a protein needed for virulence protein trafficking and provide new insights into the mechanisms for host cell remodeling, parasite survival within the host, and virulence.

Published

2020

7. Carbonate apatite nanoparticles carry siRNA(s) targeting growth factor receptor genes egfr1 and erbb2 to regress mouse breast tumor

Author

Snigdha Tiash, Nur Izyani Binti Kamaruzman, and Ezharul Hoque Chowdhury

Subjects

growth factor receptors, sirna, carbonate apatite nanoparticles (nps), gene silencing, breast cancer, tumor regression, Therapeutics. Pharmacology, RM1-950

Abstract

Cancer cells lose their control on cell cycle by numerous genetic and epigenetic alterations. In a tumor, these cells highly express growth factor receptors (GFRs), eliciting growth, and cell division. Among the GFRs, epidermal growth factor receptor-1 (EGFR1) (Her1/ERBB1) and epidermal growth factor receptor-2 (EGFR2) (Her2/ERBB2) from epidermal growth factor (EGF) family and insulin-like growth factor-1 receptor (IGF1R) are highly expressed on breast cancer cells, thus contributing to the aggressive growth and invasiveness, have been focused in this study. Moreover, overexpression of these receptors is related to suppression of cell death and conferring resistance against the classical drugs used to treat cancer nowadays. Therefore, silencing of these GFRs-encoding genes by using selective small interfering RNAs (siRNAs) could be a powerful approach to treat breast cancer. The inorganic pH sensitive carbonate apatite nanoparticles (NPs) were used as a nano-carrier to deliver siRNA(s) against single or multiple GFR genes in breast cancer cells as well as in a mouse model of breast carcinoma. Silencing of egfr1 and erbb2 simultaneously led to a reduction in cell viability with an increase in cell death signal in the cancer cells and regression of tumor growth in vivo.

Published

2017

8. siRNAs Targeting Growth Factor Receptor and Anti-Apoptotic Genes Synergistically Kill Breast Cancer Cells through Inhibition of MAPK and PI-3 Kinase Pathways

Author

Nur Izyani Kamaruzman, Snigdha Tiash, Maeirah Ashaie, and Ezharul Hoque Chowdhury

Subjects

carbonate apatite nanoparticle, siRNA, estrogen receptor (ER), mitogen-activated protein kinase (MAPK), protein kinase B (AKT), breast cancer, Biology (General), QH301-705.5

Abstract

Breast cancer, the second leading cause of female deaths worldwide, is usually treated with cytotoxic drugs, accompanied by adverse side-effects, development of chemoresistance and relapse of disease condition. Survival and proliferation of the cancer cells are greatly empowered by over-expression or over-activation of growth factor receptors and anti-apoptotic factors. Identification of these key players that cross-talk to each other, and subsequently, knockdown with their respective siRNAs in a synchronous manner could be a promising approach to precisely treat the cancer. Since siRNAs demonstrate limited cell permeability and unfavorable pharmacokinetic behaviors, pH-sensitive nanoparticles of carbonate apatite were employed to efficiently carry the siRNAs in vitro and in vivo. By delivering selective siRNAs against the mRNA transcripts of the growth factor receptors, such as ER, ERBB2 (HER2), EGFR and IGFR, and anti-apoptotic protein, such as BCL2 in human (MCF-7 and MDA-MB-231) and murine (4T1) breast cancer cell lines, we found that ESR1 along with BCL-2, or with ERBB2 and EGFR critically contributes to the growth/survival of the cancer cells by activating the MAPK and PI-3 kinase pathways. Furthermore, intravenous delivery of the selected siRNAs aiming to suppress the expression of ER/BCL2 and ER/ERBB2/EGFR groups of proteins led to a significant retardation in tumor growth in a 4T1-induced syngeneic mouse model.

Published

2018

9. Phenylbutyrate counteracts Shigella mediated downregulation of cathelicidin in rabbit lung and intestinal epithelia: a potential therapeutic strategy.

Author

Protim Sarker, Sultan Ahmed, Snigdha Tiash, Rokeya Sultana Rekha, Roger Stromberg, Jan Andersson, Peter Bergman, Gudmundur H Gudmundsson, Birgitta Agerberth, and Rubhana Raqib

Subjects

Medicine, Science

Abstract

BACKGROUND: Cathelicidins and defensins are endogenous antimicrobial peptides (AMPs) that are downregulated in the mucosal epithelia of the large intestine in shigellosis. Oral treatment of Shigella infected rabbits with sodium butyrate (NaB) reduces clinical severity and counteracts the downregulation of cathelicidin (CAP-18) in the large intestinal epithelia. AIMS: To develop novel regimen for treating infectious diseases by inducing innate immunity, we selected sodium 4-phenylbutyrate (PB), a registered drug for a metabolic disorder as a potential therapeutic candidate in a rabbit model of shigellosis. Since acute respiratory infections often cause secondary complications during shigellosis, the systemic effect of PB and NaB on CAP-18 expression in respiratory epithelia was also evaluated. METHODS: The readouts were clinical outcomes, CAP-18 expression in mucosa of colon, rectum, lung and trachea (immunohistochemistry and real-time PCR) and release of the CAP-18 peptide/protein in stool (Western blot). PRINCIPAL FINDINGS: Significant downregulation of CAP-18 expression in the epithelia of rectum and colon, the site of Shigella infection was confirmed. Interestingly, reduced expression of CAP-18 was also noticed in the epithelia of lung and trachea, indicating a systemic effect of the infection. This suggests a causative link to acute respiratory infections during shigellosis. Oral treatment with PB resulted in reduced clinical illness and upregulation of CAP-18 in the epithelium of rectum. Both PB and NaB counteracted the downregulation of CAP-18 in lung epithelium. The drug effect is suggested to be systemic as intravenous administration of NaB could also upregulate CAP-18 in the epithelia of lung, rectum and colon. CONCLUSION: Our results suggest that PB has treatment potential in human shigellosis. Enhancement of CAP-18 in the mucosal epithelia of the respiratory tract by PB or NaB is a novel discovery. This could mediate protection from secondary respiratory infections that frequently are the lethal causes in dysentery.

Published

2011

10. Structural reassignment of a dibenz[

Author

Andrew G. Riches, Christopher J. S. Hart, Matthieu Schmit, Emmanuel A. Debele, Snigdha Tiash, Erin Clapper, Tina S. Skinner-Adams, and John H. Ryan

Subjects

General Chemistry

Abstract

A screen for compounds with antigiardial activity in the Compounds Australia Scaffolds library identified SN00797640 (supplied structure being 8-acylaminodibenzoxazepinone 1) as a hit compound with potent anti-parasitic activity (concentration for 50% growth inhibition of Giardia duodenalis, IC50 0.18 μM). To further explore the structure–activity relationships in this series, compound 1 and analogues, including its 7-acylaminodibenzoxazepinone regioisomer (2), were synthesized and assessed for anti-Giardia activity. While regioisomer 2 demonstrated antigiardial activity, resynthesized 1 and other 8-acylaminodibenzoxazepinone analogues were inactive. Comparison of spectroscopic and physical properties demonstrated the correct structure of SN00797640 to be 7-acylamino regioisomer 2. These results highlight the importance of independent synthesis in verifying the structure and activity of screening hits.

Published

2022

11. An image-based Pathogen Box screen identifies new compounds with anti-Giardia activity and highlights the importance of assay choice in phenotypic drug discovery

Author

John H. Ryan, Andrew G. Riches, Snigdha Tiash, Christopher J.S. Hart, Tina S. Skinner-Adams, and Jake Saunders

Subjects

Giardiasis, 0301 basic medicine, medicine.medical_specialty, 030231 tropical medicine, Biology, Article, lcsh:Infectious and parasitic diseases, Inhibitory Concentration 50, 03 medical and health sciences, 0302 clinical medicine, Medical microbiology, Parasitic Sensitivity Tests, Prevalence, medicine, Humans, lcsh:RC109-216, Pharmacology (medical), Pathogen, Pharmacology, Antiparasitic Agents, Drug discovery, Giardia, biology.organism_classification, Virology, 3. Good health, Metronidazole, 030104 developmental biology, Infectious Diseases, Drug development, Pathogen box, Infectious disease (medical specialty), Biological Assay, Parasitology, Classical pharmacology, Giardia lamblia, Giardia duodenalis, medicine.drug

Abstract

Giardia duodenalis, the most prevalent human intestinal parasite causes the disease, giardiasis. On an annual basis G. duodenalis infects ~1 billion people, of which ~280 million develop symptomatic disease. Giardiasis can be severe and chronic, causing malnutrition, stunted growth and poor cognitive development in children. Current treatment options rely on drugs with declining efficacy and side-effects. To improve the health and well-being of millions of people world-wide, new anti-Giardia drugs with different modes of action to currently used drugs are required. The Medicines for Malaria Venture's Pathogen Box, a collection of bio-active compounds specifically chosen to stimulate infectious disease drug discovery, represents an opportunity for the discovery of new anti-Giardia agents. While the anti-Giardia activity of Pathogen Box compounds has been reported, this work failed to identify known anti-Giardia controls within the compound set. It also reported the activity of compounds previously screened and shown to be inactive by others, suggesting data may be inaccurate. Given these concerns the anti-Giardia activity of Pathogen Box compounds was re-assessed in the current study. Data from this work identified thirteen compounds with anti-Giardia IC50 values ≤2 μM. Five of these compounds were reference compounds (marketed drugs with known anti-microbial activity), or analogues of compounds with previously described anti-Giardia activity. However, eight, including MMV676358 and MMV028694, which demonstrated potent sub-μM IC50s against assemblage A, B and metronidazole resistant parasites (0.3 μM and 0.9 μM respectively), may represent new leads for future drug development. Interestingly, only four of these compounds were identified in the previously reported Pathogen Box screen highlighting the importance of assay selection and design when assessing compounds for activity against infectious agents., Graphical abstract Image 1, Highlights • 13 compounds with anti-Giardia IC50 values

Published

2020

12. Virulence determinant, PTP7, controls vesicle budding from the Maurer’s clefts, adhesin protein trafficking and host cell remodeling inPlasmodium falciparum

Author

Adam J. Blanch, Boyin Liu, Matthew W. A. Dixon, Gerald J. Shami, Olivia M. S. Carmo, Leann Tilley, Snigdha Tiash, and Dezerae Cox

Subjects

Virulence, Plasmodium falciparum, Biology, biology.organism_classification, Plasmodium, Virulence factor, Cell biology, Bacterial adhesin, Red blood cell, medicine.anatomical_structure, Cytoplasm, parasitic diseases, Organelle, medicine

Abstract

Presentation of the variant antigen,Plasmodium falciparumerythrocyte membrane protein 1 (EMP1), at knob-like protrusions on the surface of infected red blood cells, underpinsP. falciparummalaria pathogenicity. Here we describe a protein PF3D7_0301700 (PTP7), that functions at the nexus between the intermediate trafficking organelle, the Maurer’s cleft, and the infected red blood cell surface. Genetic disruption of PTP7 leads to accumulation of vesicles at the Maurer’s clefts, grossly aberrant knob morphology, and failure to deliver EMP1 to the red blood cell surface. We show that an expanded low complexity sequence in the C-terminal region of PTP7, found only in theLaveraniaclade ofPlasmodium, is critical for efficient virulence protein trafficking.Author SummaryWe describe a malaria parasite protein involved in virulence factor trafficking (PTP7) that moves between different compartments in the host red blood cell cytoplasm in a stage-dependent manner. Upon disruption of the PTP7 locus, the Maurer’s cleft trafficking compartments become decorated with vesicles; the knobby protrusions on the host red blood cell surface are depleted and distorted; and trafficking of the virulence protein, EMP1, to the host red blood cell surface is ablated. We provide evidence that a region of PTP7 with low sequence complexity plays an important role in driving fission of vesicles from the Maurer’s clefts.

Published

2021

13. siRNAs targeting multidrug transporter genes sensitise breast tumour to doxorubicin in a syngeneic mouse model

Author

Snigdha Tiash and Ezharul Hoque Chowdhury

Subjects

Small interfering RNA, ATP Binding Cassette Transporter, Subfamily B, Cell Survival, Pharmaceutical Science, Breast Neoplasms, 02 engineering and technology, Disease, Mice, 03 medical and health sciences, 0302 clinical medicine, Cell Line, Tumor, medicine, ATP Binding Cassette Transporter, Subfamily G, Member 2, Animals, Humans, Doxorubicin, Gene Silencing, RNA, Small Interfering, Gene, Mice, Inbred BALB C, Antibiotics, Antineoplastic, business.industry, technology, industry, and agriculture, Cancer, 021001 nanoscience & nanotechnology, medicine.disease, Drug Resistance, Multiple, Neoplasm Proteins, Multiple drug resistance, Drug Resistance, Neoplasm, 030220 oncology & carcinogenesis, Cancer research, Nanoparticles, Female, Efflux, Multidrug Resistance-Associated Proteins, 0210 nano-technology, business, Multidrug transporter, medicine.drug

Abstract

Chemotherapy, the commonly favoured approach to treat cancer is frequently associated with treatment failure and recurrence of disease as a result of development of multidrug resistance (MDR) with concomitant over-expression of drug efflux proteins on cancer cells. One of the most widely used drugs, doxorubicin (Dox) is a substrate of three different ATP-binding cassette (ABC) transporters, namely, ABCB1, ABCG2 and ABCC1, predominantly contributing to MDR phenotype in cancer. To silence these transporter-coding genes and thus enhance the therapeutic efficacy of Dox, pH-sensitive carbonate apatite (CA) nanoparticles (NPs) were employed as a carrier system to co-deliver siRNAs against these genes and Dox in breast cancer cells and in a syngeneic breast cancer mouse model. siRNAs and Dox were complexed with NPs by incubation at 37 °C and used to treat cancer cell lines to check cell viability and caspase-mediated signal. 4T1 cells-induced breast cancer mouse model was used for treatment with the complex to confirm their action in tumour regression. Smaller (∼200 nm) and less polydisperse NPs that were taken up more effectively by tumour tissue could enhance Dox chemosensitivity, significantly reducing the tumour size in a very low dose of Dox (0.34 mg/kg), in contrast to the limited effect observed in breast cancer cell lines. The study thus proposes that simultaneous delivery of siRNAs against transporter genes and Dox with the help of CA NPs could be a potential therapeutic intervention in effectively treating MDR breast cancer.

Published

2019

14. Improved DNA delivery using invasive E. coli DH10B in human cells by modified bactofection method

Author

Snigdha Tiash and Alviya Sultana

Subjects

Genetic Vectors, Pharmaceutical Science, 02 engineering and technology, Gene delivery, Transfection, Green fluorescent protein, Viral vector, HeLa, 03 medical and health sciences, Escherichia coli, Humans, 030304 developmental biology, 0303 health sciences, Reporter gene, biology, Chemistry, Escherichia coli Proteins, Gene Transfer Techniques, DNA, 021001 nanoscience & nanotechnology, Entry into host, biology.organism_classification, Cell biology, Cell culture, 0210 nano-technology, Bacterial Outer Membrane Proteins

Abstract

E. coli mediated gene delivery faces a major drawback of low efficiency despite of being a safer alternative to viral vectors. This study showed a novel, simple and effective strategy to enhance invasive E. coli DH10B vector's efficiency in human epithelial cells. The bactofection efficiency of invasive E .coli vector was analyzed in nine cell lines. It demonstrated highest (16%) reporter gene (GFP) expression in cervical cells. Methods were employed to further enhance its efficiency by adding transfection reagents (trans-bactofection method) to promote entry into host cells, lysosomotropic reagents for escape from lysosomal degradation or antibiotics to lyse internalized bacteria. Increased bacterial entry, as elucidated from nil to 3% expression in liver cells, was obtained upon complexing bacteria with PULSin. Chloroquine mediated endosomal escape resulted in 7.2 folds increase whereas tetracycline addition to lyse internalized bacteria caused ≈90% of GFP in HeLa. Eventually, the combined effect of these three methods exhibited close to 100% GFP in cervical and remarkable increase of 138 folds in breast cells. This is the first study showing comparative study of vector's gene delivery ability in various epithelial cells of the human body with improving its delivery efficiency. These data demonstrated the potential of developed bactofection method to boost up the efficiency of other bacterial vectors also, which could further be used for effectual therapeutic gene delivery in human cells.

Published

2020

15. Surface area-to-volume ratio, not cellular rigidity, determines red blood cell traversal through small capillaries

Author

Matthew W. A. Dixon, Oliver Looker, Peter Vee Sin Lee, Olivia M. S. Carmo, Arman Namvar, Li-Jin Chan, Leann Tilley, Dean Andrew, Wai-Hong Tham, Vijay Rajagopal, Adam J. Blanch, Snigdha Tiash, and Boyin Liu

Subjects

Red blood cell, Rigidity (electromagnetism), medicine.anatomical_structure, Membrane, Surface-area-to-volume ratio, Chemistry, Biophysics, medicine, Marked effect, Rbc membrane, Viscoelasticity, circulatory and respiratory physiology

Abstract

SummaryThe remarkable deformability of red blood cells (RBCs) depends on the viscoelasticity of the plasma membrane and cell contents and the surface area to volume (SA:V) ratio; however, it remains unclear which of these factors is the key determinant for passage through small capillaries. We used a microfluidic device to examine the traversal of normal, stiffened, swollen, parasitised and immature RBCs. We show that dramatic stiffening of RBCs had no measurable effect on their ability to traverse small channels. By contrast, a moderate decrease in the SA:V ratio had a marked effect on the equivalent cylinder diameter that is traversable by RBCs of similar stiffness. We developed a finite element model that provides a coherent rationale for the experimental observations, based on the nonlinear mechanical behaviour of the RBC membrane skeleton. We conclude that the SA:V ratio should be given more prominence in studies of RBC pathologies.

Published

2020

16. Surface area-to-volume ratio, not cellular viscoelasticity, is the major determinant of red blood cell traversal through small channels

Author

Oliver Looker, Matthew W. A. Dixon, Peter Vee Sin Lee, Leann Tilley, Snigdha Tiash, Vijay Rajagopal, Arman Namvar, Adam J. Blanch, Olivia M. S. Carmo, Wai-Hong Tham, Boyin Liu, Li-Jin Chan, and Dean Andrew

Subjects

Erythrocytes, Immunology, red blood cell, Biology, Microbiology, Models, Biological, Viscoelasticity, Microcirculation, 03 medical and health sciences, Reticulocyte, Cell Movement, Virology, Erythrocyte Deformability, Lab-On-A-Chip Devices, medicine, Cylinder, Erythrocyte deformability, Humans, deformability, Cell Shape, Research Articles, 030304 developmental biology, Cell Size, 0303 health sciences, 030306 microbiology, reticulocyte, hemic and immune systems, Capillaries, Red blood cell, Membrane, medicine.anatomical_structure, Surface-area-to-volume ratio, plasmodium, Biophysics, surface area‐to‐volume ratio, circulatory and respiratory physiology, Research Article

Abstract

The remarkable deformability of red blood cells (RBCs) depends on the viscoelasticity of the plasma membrane and cell contents and the surface area to volume (SA:V) ratio; however, it remains unclear which of these factors is the key determinant for passage through small capillaries. We used a microfluidic device to examine the traversal of normal, stiffened, swollen, parasitised and immature RBCs. We show that dramatic stiffening of RBCs had no measurable effect on their ability to traverse small channels. By contrast, a moderate decrease in the SA:V ratio had a marked effect on the equivalent cylinder diameter that is traversable by RBCs of similar cellular viscoelasticity. We developed a finite element model that provides a coherent rationale for the experimental observations, based on the nonlinear mechanical behaviour of the RBC membrane skeleton. We conclude that the SA:V ratio should be given more prominence in studies of RBC pathologies.

Published

2020

17. Role of <named-content content-type='genus-species'>Plasmodium falciparum</named-content> Protein GEXP07 in Maurer’s Cleft Morphology, Knob Architecture, and <named-content content-type='genus-species'>P. falciparum</named-content> EMP1 Trafficking

Author

Oliver Looker, Matthew W. A. Dixon, Andy J. Y. Low, Emma McHugh, Olivia M. S. Carmo, Boyin Liu, Adam J. Blanch, Steven Batinovic, Dean Andrew, Snigdha Tiash, Hyun-Jung Cho, Paul J. McMillan, and Leann Tilley

Subjects

Erythrocytes, Plasmodium falciparum, Protozoan Proteins, malaria, Virulence, Microbiology, Green fluorescent protein, Cell Line, Host-Parasite Interactions, Host-Microbe Biology, 03 medical and health sciences, Antigen, Virology, Organelle, parasitic diseases, Humans, Protein Interaction Maps, 030304 developmental biology, 0303 health sciences, biology, 030306 microbiology, Erythrocyte Membrane, Membrane Proteins, Maurer's cleft, biology.organism_classification, QR1-502, 3. Good health, Transport protein, Cell biology, Protein Transport, Membrane protein, protein trafficking, Carrier Proteins, virulence determinants, Research Article

Abstract

The trafficking of the virulence antigen PfEMP1 and its presentation at the knob structures at the surface of parasite-infected RBCs are central to severe adhesion-related pathologies such as cerebral and placental malaria. This work adds to our understanding of how PfEMP1 is trafficked to the RBC membrane by defining the protein-protein interaction networks that function at the Maurer’s clefts controlling PfEMP1 loading and unloading. We characterize a protein needed for virulence protein trafficking and provide new insights into the mechanisms for host cell remodeling, parasite survival within the host, and virulence., The malaria parasite Plasmodium falciparum traffics the virulence protein P. falciparum erythrocyte membrane protein 1 (PfEMP1) to the surface of infected red blood cells (RBCs) via membranous organelles, known as the Maurer’s clefts. We developed a method for efficient enrichment of Maurer’s clefts and profiled the protein composition of this trafficking organelle. We identified 13 previously uncharacterized or poorly characterized Maurer’s cleft proteins. We generated transfectants expressing green fluorescent protein (GFP) fusions of 7 proteins and confirmed their Maurer’s cleft location. Using co-immunoprecipitation and mass spectrometry, we generated an interaction map of proteins at the Maurer’s clefts. We identified two key clusters that may function in the loading and unloading of PfEMP1 into and out of the Maurer’s clefts. We focus on a putative PfEMP1 loading complex that includes the protein GEXP07/CX3CL1-binding protein 2 (CBP2). Disruption of GEXP07 causes Maurer’s cleft fragmentation, aberrant knobs, ablation of PfEMP1 surface expression, and loss of the PfEMP1-mediated adhesion. ΔGEXP07 parasites have a growth advantage compared to wild-type parasites, and the infected RBCs are more deformable and more osmotically fragile.

Published

2020

18. Carbonate apatite nanoparticles carry siRNA(s) targeting growth factor receptor genes egfr1 and erbb2 to regress mouse breast tumor

Author

Snigdha Tiash, Ezharul Hoque Chowdhury, and Nur Izyani Kamaruzman

Subjects

0301 basic medicine, Cell Survival, Receptor, ErbB-2, tumor regression, Pharmaceutical Science, Breast Neoplasms, carbonate apatite nanoparticles (nps), RM1-950, Biology, Growth Factor Receptor Gene, Mice, gene silencing, 03 medical and health sciences, sirna, breast cancer, 0302 clinical medicine, Growth factor receptor, Epidermal growth factor, Apatites, Cell Line, Tumor, medicine, Animals, Humans, RNA, Small Interfering, growth factor receptors, skin and connective tissue diseases, Cell Proliferation, Insulin-like growth factor 1 receptor, Mice, Inbred BALB C, Cell Death, Epidermal Growth Factor, Cell growth, Cancer, General Medicine, Cell cycle, medicine.disease, Molecular biology, ErbB Receptors, 030104 developmental biology, 030220 oncology & carcinogenesis, Cancer cell, MCF-7 Cells, Cancer research, Nanoparticles, Female, Therapeutics. Pharmacology, Research Article, Signal Transduction

Abstract

Cancer cells lose their control on cell cycle by numerous genetic and epigenetic alterations. In a tumor, these cells highly express growth factor receptors (GFRs), eliciting growth, and cell division. Among the GFRs, epidermal growth factor receptor-1 (EGFR1) (Her1/ERBB1) and epidermal growth factor receptor-2 (EGFR2) (Her2/ERBB2) from epidermal growth factor (EGF) family and insulin-like growth factor-1 receptor (IGF1R) are highly expressed on breast cancer cells, thus contributing to the aggressive growth and invasiveness, have been focused in this study. Moreover, overexpression of these receptors is related to suppression of cell death and conferring resistance against the classical drugs used to treat cancer nowadays. Therefore, silencing of these GFRs-encoding genes by using selective small interfering RNAs (siRNAs) could be a powerful approach to treat breast cancer. The inorganic pH sensitive carbonate apatite nanoparticles (NPs) were used as a nano-carrier to deliver siRNA(s) against single or multiple GFR genes in breast cancer cells as well as in a mouse model of breast carcinoma. Silencing of egfr1 and erbb2 simultaneously led to a reduction in cell viability with an increase in cell death signal in the cancer cells and regression of tumor growth in vivo.

Published

2020

19. Multimodal analysis of Plasmodium knowlesi ‐infected erythrocytes reveals large invaginations, swelling of the host cell, and rheological defects

Author

Eric Hanssen, Leann Tilley, Adam J. Blanch, Vijay Rajagopal, Matthew W. A. Dixon, Dean Andrew, Olivia M. S. Carmo, Arman Namvar, Snigdha Tiash, and Boyin Liu

Subjects

Cytoplasm, Erythrocytes, Lysis, Plasmodium falciparum, Schizonts, Immunology, Vacuole, Microbiology, Host-Parasite Interactions, Hemoglobins, 03 medical and health sciences, Osmotic Pressure, Virology, Humans, Plasmodium knowlesi, Trophozoites, Research Articles, 030304 developmental biology, 0303 health sciences, biology, Merozoites, 030306 microbiology, Vesicle, Erythrocyte Membrane, biology.organism_classification, 3. Good health, Cell biology, Vacuoles, Host cell cytoplasm, Microscopy, Electron, Scanning, Ultrastructure, Research Article

Abstract

The simian parasite Plasmodium knowlesi causes severe and fatal malaria infections in humans, but the process of host cell remodelling that underpins the pathology of this zoonotic parasite is only poorly understood. We have used serial block‐face scanning electron microscopy to explore the topography of P. knowlesi‐infected red blood cells (RBCs) at different stages of asexual development. The parasite elaborates large flattened cisternae (Sinton Mulligan's clefts) and tubular vesicles in the host cell cytoplasm, as well as parasitophorous vacuole membrane bulges and blebs, and caveolar structures at the RBC membrane. Large invaginations of host RBC cytoplasm are formed early in development, both from classical cytostomal structures and from larger stabilised pores. Although degradation of haemoglobin is observed in multiple disconnected digestive vacuoles, the persistence of large invaginations during development suggests inefficient consumption of the host cell cytoplasm. The parasite eventually occupies ~40% of the host RBC volume, inducing a 20% increase in volume of the host RBC and an 11% decrease in the surface area to volume ratio, which collectively decreases the ability of the P. knowlesi‐infected RBCs to enter small capillaries of a human erythrocyte microchannel analyser. Ektacytometry reveals a markedly decreased deformability, whereas correlative light microscopy/scanning electron microscopy and python‐based skeleton analysis (Skan) reveal modifications to the surface of infected RBCs that underpin these physical changes. We show that P. knowlesi‐infected RBCs are refractory to treatment with sorbitol lysis but are hypersensitive to hypotonic lysis. The observed physical changes in the host RBCs may underpin the pathology observed in patients infected with P. knowlesi.

Published

2019

20. Surface Area-to-Volume Ratio, not Cellular Viscoelasticity is the Major Determinant of Red Blood Cell Traversal through Small Channels

Author

Peter Vee Sin Lee, Matthew W. A. Dixon, Leann Tilley, Arman Namvar, Boyin Liu, Oliver Looker, Vijay Rajagopal, Olivia M. S. Carmo, Wai-Hong Tham, Snigdha Tiash, Adam J. Blanch, Li-Jin Chan, and Dean Andrew

Subjects

Chemistry, Biophysics, hemic and immune systems, Marked effect, Rbc membrane, Viscoelasticity, Red blood cell, Membrane, medicine.anatomical_structure, Surface-area-to-volume ratio, medicine, Cylinder, circulatory and respiratory physiology

Abstract

The remarkable deformability of red blood cells (RBCs) depends on the viscoelasticity of the plasma membrane and cell contents and the surface area to volume (SA:V) ratio; however, it remains unclear which of these factors is the key determinant for passage through small capillaries. We used a microfluidic device to examine the traversal of normal, stiffened, swollen, parasitised and immature RBCs. We show that dramatic stiffening of RBCs had no measurable effect on their ability to traverse small channels. By contrast, a moderate decrease in the SA:V ratio had a marked effect on the equivalent cylinder diameter that is traversable by RBCs of similar cellular viscoelasticity. We developed a finite element model that provides a coherent rationale for the experimental observations, based on the nonlinear mechanical behaviour of the RBC membrane skeleton. We conclude that the SA:V ratio should be given more prominence in studies of RBC pathologies.

Published

2021

21. Knockdown of ROS1 gene sensitizes breast tumor growth to doxorubicin in a syngeneic mouse model

Author

Snigdha Tiash, Ezharul Hoque Chowdhury, and Ming Jang Chua

Subjects

0301 basic medicine, Cancer Research, Paclitaxel, Biology, Mice, Phosphatidylinositol 3-Kinases, Random Allocation, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Breast cancer, Apatites, Cell Line, Tumor, Proto-Oncogene Proteins, medicine, Animals, Gene silencing, Doxorubicin, RNA, Small Interfering, Mice, Inbred BALB C, Gene knockdown, Oncogene, Mammary Neoplasms, Experimental, Receptor Protein-Tyrosine Kinases, Cancer, Drug Synergism, medicine.disease, 030104 developmental biology, Oncology, chemistry, Gene Knockdown Techniques, 030220 oncology & carcinogenesis, Cancer cell, Cancer research, Female, Cisplatin, Proto-Oncogene Proteins c-akt, medicine.drug

Abstract

Treatment of breast cancer, the second leading cause of female deaths worldwide, with classical drugs is often accompanied by treatment failure and relapse of disease condition. Development of chemoresistance and drug toxicity compels compromising the drug concentration below the threshold level with the consequence of therapeutic inefficacy. Moreover, amplification and over-activation of proto-oncogenes in tumor cells make the treatment more challenging. The oncogene, ROS1 which is highly expressed in diverse types of cancers including breast carcinoma, functions as a survival protein aiding cancer progression. Thus we speculated that selective silencing of ROS1 gene by carrier-mediated delivery of siRNA might sensitize the cancer cells to the classical drugs at a relatively low concentration. In this investigation we showed that intracellular delivery of c-ROS1-targeting siRNA using pH-sensitive inorganic nanoparticles of carbonate apatite sensitizes mouse breast cancer cells (4T1) to doxorubicin, but not to cisplatin or paclitaxel, with the highest enhancement in chemosensitivity obtained at 40 nM of the drug concentration. Although intravenous administrations of ROS1-loaded nanoparticles reduced growth of the tumor, a further substantial effect on growth retardation was noted when the mice were treated with the siRNA- and Dox-bound particles, thus suggesting that silencing of ROS1 gene could sensitize the mouse breast cancer cells both in vitro and in vivo to doxorubicin as a result of synergistic effect of the gene knockdown and the drug action, eventually preventing activation of the survival pathway protein, AKT1. Our findings therefore provide valuable insight into the potential cross-talk between the pathways of ROS1 and doxorubicin for future development of effective therapeutics for breast cancer.

Published

2016

22. Methotrexate- and Cyclophosphamide-embedded Pure and Strontiumsubstituted Carbonate Apatite Nanoparticles for Augmentation of Chemotherapeutic Activities in Breast Cancer Cells

Author

Iekhsan Othman, Rosita Rosli, Snigdha Tiash, and Ezharul Hoque Chowdhury

Subjects

Antimetabolites, Antineoplastic, Cyclophosphamide, Cell Survival, Pharmaceutical Science, Breast Neoplasms, Pharmacology, Apatite, Apatites, medicine, Humans, Viability assay, Chemistry, Methotrexate, Strontium, visual_art, Cancer cell, Toxicity, MCF-7 Cells, visual_art.visual_art_medium, Nanoparticles, Female, Efflux, Nanocarriers, medicine.drug

Abstract

Most of the classical drugs used today to destroy cancer cells lead to the development of acquired resistance in those cells by limiting cellular entry of the drugs or exporting them out by efflux pumps. As a result, higher doses of drugs are usually required to kill the cancer cells affecting normal cells and causing numerous side effects. Accumulation of the therapeutic level of drugs inside the cancer cells is thus required for an adequate period of time to get drugs' complete therapeutic efficacy minimizing the side effects on normal cells. In order to improve the efficacy of chemotherapeutic drugs, nanoparticles of carbonate apatite and its strontium (Sr(2+))-substituted derivative were used in this study to make complexes with three classical anticancer drugs, methotrexate, cyclophosphamide and 5-flurouracil. The binding affinities of these drugs to apatite were evaluated by absorbance and HPLC analysis and the therapeutic efficacy of drug-apatite complexes was determined by cell viability assay. Carbonate apatite demonstrated significant binding affinity towards methotrexate and cyclophosphamide leading to more cellular toxicity than free drugs in MCF-7 and 4T1 breast cancer cells. Moreover, Sr(2+) substitution in carbonate apatite with resulting tiny particles less than 100 nm in diameter further promoted binding of methotrexate to the nanocarriers indicating that Sr(2+)-substituted apatite nanoparticles have the high potential for loading substantial amount of anti-cancer drugs with eventual more therapeutic effectiveness.

Published

2014

23. Treatment with phenylbutyrate in a pre-clinical trial reduces diarrhea due to enteropathogenic Escherichia coli: link to cathelicidin induction

Author

Snigdha Tiash, Gudmundur H. Gudmundsson, Mahmuda Akter, Alejandro Cravioto, Birgitta Agerberth, Kaisar A. Talukder, Armadno Navarro, Protim Sarker, Abdullah Al-Mamun, Akhirunnessa Mily, Rubhana Raqib, and M. Islam

Subjects

Diarrhea, Shigellosis, medicine.medical_treatment, Immunology, Administration, Oral, Virulence, Biology, Microbiology, Phenylbutyrate, Cathelicidin, Enteropathogenic Escherichia coli, Feces, Western blot, Cathelicidins, Intestine, Small, medicine, Animals, Immunologic Factors, Escherichia coli Infections, Bacterial Shedding, medicine.diagnostic_test, Gene Expression Profiling, medicine.disease, Phenylbutyrates, Small intestine, Disease Models, Animal, Treatment Outcome, Infectious Diseases, medicine.anatomical_structure, Rabbits, medicine.symptom, Antimicrobial Cationic Peptides

Abstract

Treatment of shigellosis in rabbits with phenylbutyrate reduces clinical severity and counteracts down-regulation of cathelicidin (CAP-18) in the large intestinal epithelia. We aimed to further evaluate whether in a rabbit model of enteropathogenic Escherichia coli (EPEC) diarrhea, CAP-18 is down-regulated in the small intestine and if oral phenylbutyrate treatment affects CAP-18 expression, clinical recovery, shedding of EPEC in stool and virulence properties of the isolated colonies. EPEC-induced diarrhea down-regulated CAP-18 in the small intestinal epithelia as revealed by immunohistochemistry. Phenylbutyrate treatment reduced clinical illness, improved histological features of inflammation and up-regulated CAP-18 in the epithelia. Active CAP-18 peptide was also released in the stool as noted in Western blot analysis. Multiplex PCR analysis of total bacterial DNA in the stool showed absence of EPEC specific genes eae and bfpA. Treated rabbits shed rough strains still harboring eae and bfpA genes, which were less potent in binding to HeLa cells and induced delayed onset of diarrhea in new rabbits. In conclusion, EPEC-mediated down-regulation of CAP-18 in the small intestinal epithelia was restored by phenylbutyrate treatment. Upregulation of CAP-18 in the epithelia was accompanied by healing of the epithelial lining, reduced shedding and virulence of EPEC and recovery from diarrhea.

Published

2013

24. Passive Targeting of Cyclophosphamide-Loaded Carbonate Apatite Nanoparticles to Liver Impedes Breast Tumor Growth in a Syngeneic Model

Author

Ezharul Hoque Chowdhury and Snigdha Tiash

Subjects

0301 basic medicine, Cyclophosphamide, Cell Survival, medicine.medical_treatment, Antineoplastic Agents, Breast Neoplasms, 02 engineering and technology, 03 medical and health sciences, Mice, Breast cancer, Apatites, Drug Discovery, medicine, Distribution (pharmacology), Animals, Prodrugs, Particle Size, Cytotoxicity, Cell Proliferation, Pharmacology, Chemotherapy, Mice, Inbred BALB C, Chemistry, Cell growth, Cancer, Prodrug, 021001 nanoscience & nanotechnology, medicine.disease, Disease Models, Animal, 030104 developmental biology, Liver, Immunology, Cancer research, Nanoparticles, Female, 0210 nano-technology, medicine.drug

Abstract

Despite being widely used for treating cancer, chemotherapy is accompanied by numerous adverse effects as a result of systemic distribution and nonspecific interactions of the drugs with healthy tissues, eventually leading to therapeutic inefficacy and chemoresistance. Cyclophosphamide (Cyp) as one of the chemotherapeutic pro-drugs is activated in liver and used to treat breast cancer in high dose and in combination with other drugs. In an attempt to reduce the off-target effects and enhance the therapeutic efficacy, pH-sensitive carbonate apatite nanoparticles that had predominantly and size-dependently been localized in liver following intravenous administration, were employed to electrostatically immobilize Cyp and purposely deliver it to the liver for activation. Cyp-loaded particles formed by simple 30 min incubation at 37oC of the DMEM (pH 7.4) medium containing CaCl2 and Cyp, enhanced in vitro cytotoxicity at different degrees depending on the cell types. The size of the particles could be tightly controlled by the amount of CaCl2 required to prepare the particles and thus the bio-distribution pattern inside different organs of the body. Unlike the small particles (~ 200 nm), the large size particles (~ 600 nm) which were more efficiently accumulated in liver, significantly reduced the tumor volume following intravenous injection in 4T1-induced murine breast cancer model at a very low dose (0.17 mg/Kg) of the drug initially added for complex formation, thus shedding light on the potential applications of the Cyp-loaded nano-formulations in the treatment of breast cancer.

Published

2015

25. Knockdown of PLC-gamma-2 and calmodulin 1 genes sensitizes human cervical adenocarcinoma cells to doxorubicin and paclitaxel

Author

Diyana Salleh, Tahereh Fatemian, Ezharul Hoque Chowdhury, Snigdha Tiash, Toshihiro Akaike, Anthony Stanislaus, Sharif Hossain, and Athirah Bakhtiar

Subjects

Cancer Research, Small interfering RNA, Paclitaxel, PLC-gamma-2, Pharmacology, Endocytosis, lcsh:RC254-282, Calmodulin 1, Nanoparticle, RNA interference, Gene expression, Genetics, Medicine, Doxorubicin, lcsh:QH573-671, Cisplatin, Gene knockdown, business.industry, lcsh:Cytology, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Oncology, Carbonate apatite, siRNA, Cancer research, Cervical cancer, business, Primary Research, medicine.drug

Abstract

Background RNA interference (RNAi) is a powerful approach in functional genomics to selectively silence messenger mRNA (mRNA) expression and can be employed to rapidly develop potential novel drugs against a complex disease like cancer. However, naked siRNA being anionic is unable to cross the anionic cell membrane through passive diffusion and therefore, delivery of siRNA remains a major hurdle to overcome before the potential of siRNA technology can fully be exploited in cancer. pH-sensitive carbonate apatite has recently been developed as an efficient tool to deliver siRNA into the mammalian cells by virtue of its high affinity interaction with the siRNA and the desirable size distribution of the resulting siRNA-apatite complex for effective cellular endocytosis. Moreover, internalized siRNA was found to escape from the endosomes in a time-dependent manner and efficiently silence gene expression. Results Here we show that carbonate apatite-mediated delivery of siRNA against PLC-gamma-2 (PLCG2) and calmodulin 1 (CALM1) genes has led to the sensitization of a human cervical cancer cell line to doxorubicin- and paclitaxel depending on the dosage of the individual drug whereas no such enhancement in cell death was observed with cisplatin irrespective of the dosage following intracellular delivery of the siRNAs. Conclusion Thus, PLCG2 and CALM1 genes are two potential targets for gene knockdown in doxorubicin and paclitaxel-based chemotherapy of cervical cancer.

Published

2012

26. Growth factor receptors: promising drug targets in cancer

Author

Ezharul Hoque Chowdhury and Snigdha Tiash

Subjects

Small interfering RNA, medicine.drug_class, Angiogenesis, Cancer, Biology, Pharmacology, medicine.disease, Tyrosine-kinase inhibitor, Metastasis, Oncology, Growth factor receptor, Cancer cell, medicine, Nanocarriers

Abstract

Genetic, epigenetic and somatic changes deregulate the expression of growth factor receptors (GFRs), leading to cancer initiation and progression. Tumor cell growth and survival are orchestrated by clonal expansion and evasion of apoptotic signals in cancer cells. The growth of cells is further supported by angiogenesis and metastasis to distant organs. High expression of GFRs also contributes to the development of resistance. Therefore, therapeutics to target GFRs is a potentially attractive molecular approach to treat cancer more effectively. In this review, we have discussed the contribution of GFRs to cancer development and addressed molecular approaches undertaken to inhibit GFR-mediated pathways. A wide number of monoclonal antibodies (mAbs) and protein kinase inhibitors targeting these GFR-mediated functions are in clinical trials to treat human malignancies. However, most drugs that target GFRs lead to the development of drug resistance and generate adverse effects. Nucleic acid-based therapeutics, e.g. short interfering RNA (siRNA) could be harnessed to selectively silence GFR genes in cancer cells. Different polymer, liposome-based nanocarriers, and the most recently developed pH-sensitive inorganic carbonate apatite nanoparticles have been used in cell culture and preclinical trials for cytoplasmic delivery of the siRNAs targeting different GFR genes. siRNA-based therapeutics have been shown to have significant potential to suppress GFR expression and functions and thus could be developed as molecular therapeutics. Multi-targeting of tumors at different levels by combining various approaches along with chemotherapy would be a promising therapeutic approach to fight the disease. Suitable nanocarriers capable of entrapping siRNA, mAb, GFR inhibitors and classical drugs targeting GFR have potential therapeutic applications.

Published

2015