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Antiviral API
- Arenavirus
- Cytomegalovirus (CMV)
- Dengue virus
- Endogenous Metabolite
- Enterovirus (EV)
- Epstein-Barr virus (EBV)
- Filovirus
- Flavivirus
- HCV Protease
- Hepatitis B Virus (HBV)
- Hepatitis C Virus (HCV)
- Herpes simplex Virus (HSV)
- HIF/HIF Prolyl-Hydroxylase
- HIV Integrase
- HIV Protease
- Human immunodeficiency Virus (HIV)
- Human papillomavirus (HPV)
- Influenza Virus
- Nipah virus
- Orthopoxvirus
- Others
- Rabies virus (RABV)
- Respiratory syncytial Virus (RSV)
- Reverse Transcriptases (RTs)
- SARS-CoV
- Tobacco mosaic virus (TMV)
- Vesicular stomatitis virus (VSV)
- Virus Protease
- West Nile virus
- Antiviral intermediates
Dengue virus
CAS No. | Product Name | Inquiry |
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1469988-75-7 |
QL47QL47 is a potent and selective BTK inhibitor, which covalently modifies Cys481. QL47 inhibits BTK kinase activity with an IC50 of 7 nM, inhibits autophosphorylation of BTK on Tyr223 in cells with an EC50 of 475 nM and inhibits phosphorylation of a downstream effector PLCγ2 (Tyr759) with an EC50 of 318 nM. In Ramos cells QL47 induces a G1 cell cycle arrest which is associated with pronounced degradation of BTK protein. QL47 inhibits the proliferation of B-cell lymphoma cancer cell lines at submicromolar concentrations. |
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1809464-07-0 |
DENV-IN-8 |
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19956-53-7 |
LucidoneLucidone, coming from the root of Lindera strychnifolia, may possess antioxidant and anti-inflammatory properties and may be useful for the prevention of free radical-induced skin damage. The anti-inflammatory activity of lucidone might cause by the inhibition of iNOS and COX-2 expressions through the down-regulation of NF-κB and AP-1 binding activity. Besides, the effects of lucidone on tyrosinase and antimelanogenic activity were investigated, lucidone strongly inhibits the activity of mushroom tyrosinase. The antimelanogenic activity of lucidone is probably due to its inhibition of tyrosinase activity and the suppression of tyrosinase and MITF expression. |
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2043343-94-6 |
Mosnodenvir |
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2165969-58-2 |
Antiviral agent 51 |
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2253675-62-4 |
Denv-IN-2 |
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2361289-44-1 |
Chikv-IN-2 |
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2375781-06-7 |
DENV-IN-5DENV-IN-5 is a dengue virus (DENV) inhibitor with EC50s of 1.47, 9.23, 7.08 and 8.91 μM against DENV-I - IV replication, respectively. DENV-IN-5 also inhibits HIV-1IIIB strain with an EC50 of 0.1512 μM. |
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2396706-31-1 |
GAK inhibitor 2 |
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2407227-31-8 |
NITD-688NITD-688 is an orally active panserotype inhibitor of dengue virus NS4B protein that can be used in dengue virus (DENV) studies. |
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24280-93-1 |
Mycophenolic AcidMycophenolic acid is a small lactone antibiotic produced by Pen. brevicom pactum and Pen. stoloniferum. Activity against gram-positive bacteria. In animal experiments, it has inhibitory effect on sarcoma-180, Lewis lung cancer, adenocarcinoma Ca-755, Walker tumor 256, Yoshida sarcoma, Freund ascites tumor, etc. Mycophenolic acid is a potent IMPDH inhibitor and the active metabolite of an immunosuppressive drug, used to prevent rejection in organ transplantation. It inhibits an enzyme needed for the growth of T cells and B cells. |
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2499537-22-1 |
Denv-IN-7 |
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2581065-80-5 |
DENV-IN-12 |
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29066-42-0 |
HymeglusinIt is a β-lactone antibiotic produced by the strain of Cephalosporium sp. It has a strong inhibitory effect on hydroxymethyl glutaryl coenzyme A (HMG-CoA) synthase. |
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3010940-08-3 |
NS2B/NS3-IN-2 |
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37415-62-6 |
Mycophenolic acid sodiumMycophenolate Sodium, a mcophenolic acid derivative, is used as an immunosuppressive agent in organ transplantation and autoimmune diseases. |
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390803-40-4 |
ST-148 maleateST 148 is a dopamine D2 receptor antagonist. |
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587841-73-4 |
ZCL278ZCL 278 is a cell-permeable inhibitor of Cdc42, a Rho family GTPase. It binds into the surface groove on Cdc42 (Kd = 6.4-11.4 µM), blocking interaction with intersectin (ITSN), a guanine nucleotide exchange factor (GEF). |
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60-93-5 |
Quinine dihydrochloride |
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480-41-1 |
NaringeninNaringenin is a natural predominant flavanone derived from plant food with antioxidant and anti-inflammatory activity. Naringenin reduces oxidative damage to DNA in vitro, and increases VLDL as well as cholesterol levels. Naringenin is used for the treatment of HCV infection. Naringenin can be used as nutritional supplement in health care products. |
What is Dengue virus (DENV)?
Dengue virus (DENV) belongs to the genus Flaviviridae and is transmitted to humans by Aedes mosquitoes, mainly Aedes Egypt. Dengue virus can be classified into four types: DENV-1, DENV-2, DENV-3 and DENV-4. Dengue virus infection is the leading cause of disease in tropical and subtropical regions, with an estimated 50 million infections each year and more than 2.5 billion people at risk of infection.
Mature DENV virions are characterized by a smooth surface with a diameter of about 50 nM, while immature virions are 60 nm in diameter with spikes on the surface. The genome encodes 3 structural proteins (capsid (C, 100 amino acids (aa)), anterior membrane/membrane (prM/M, 75 aa (and envelope (E, 495 aa)), and 7 non-structural proteins (NS1, NS2A, NS2B, NS3, NS4A, NS4B, and NS5). Structural proteins form the building blocks of DENV virions, while nonstructural proteins are involved in RNA replication.
Fig.1 Genome structure of Dengue virus. (Siritt Maria Eugenia Guzman, et al., 2010)
How did the Dengue virus spread?
After the Aedes mosquito bites a dengue fever patient or a latently infected person, the dengue virus generally needs to multiply in the body of the Aedes mosquito after 8~10 days, and the dengue virus can be transmitted to healthy people through the bite. However, it is important to note that the dengue virus is not transmitted directly from person to person.
Dengue virus diseases
Latent infection, dengue fever and dengue hemorrhagic fever may occur after the dengue virus infects the human body. Clinically, dengue fever can be divided into typical, mild and severe, and in patients with severe dengue, the mortality rate can be as high as 50%. Typical dengue fever has the following symptoms: fever, which usually begins suddenly, and the body temperature rises rapidly above 39 degrees Celsius, usually lasting 2 to 7 days. The rash appears 2 to 5 days after onset, initially on the palms, soles of the feet, or trunk and abdomen, and gradually extends to the neck and limbs. Bleeding occurs 5 to 8 days after onset, and about half of cases may have bleeding of varying degrees from different locations. In addition, the lymph nodes throughout the body may be mildly enlarged with mild tenderness.
Dengue virus test
DENV infection can be diagnosed directly by testing for viral components in serum or indirectly by serological methods. The sensitivity of the various methods depends on the duration of the disease and at what stage of the course the patient is being evaluated. Detection of viral nucleic acids or viral antigens is more specific, but more cumbersome and expensive. Serologic testing is less specific, but it is easier to perform and less expensive.
IgM can be detected as early as 4 days after onset by lateral flow immunoassay or IgM antibody capture ELISA. In addition, isolation of the virus (culture method) can also confirm DENV infection, and in general, culture methods are not necessary for clinical diagnosis, as culture results are usually not available within a clinically meaningful time frame. Immunohistochemical staining can detect DENV protein in tissue samples, and the detection rate appears to be higher in liver tissue.
Dengue virus treatment
Dengue virus vaccines
At present, there are three main dengue vaccines in the leading state of research and development, namely Dengvaxia (CYD-TDV) (Sanofi Pasteur of France), Qdenga (TAK-003) (Takeda Pharmaceutical of Japan), and TV003 (National Institutes of Health of United States).
Denvaxia is currently the only vaccine licensed in multiple countries and the first to be included in the World Health Organization's prequalification vaccine list. However, the vaccine has been observed to be less effective and less effective in children and dengue patients, and it also increases the risk of severe dengue fever in people who have not been infected with dengue after vaccination.
The results of the Phase 3 clinical trial of TAK-003 (DENVax) have been released, which can produce a good immune effect and reduce the incidence of severe disease. The World Health Organization (WHO) announced on 15 May 2024 that TAK-003 (DENVax) vaccine has been added to the WHO Prequalification List of vaccines recommended for children aged 6 to 16 years in areas with high levels of dengue virus transmission. The vaccine is given in two doses, 3 months apart.
The phase III clinical trial of TV-003/TV-005 (LATV) vaccine showed that the vaccine can produce better immune effects and reduce the incidence of severe disease.
Dengue virus medicine therapy
The development of small molecule anti-dengue drugs has been a slow process. To date, there are only four small-molecule anti-dengue drugs: Chloroquine (NCT00849602), Celgosivir (NCT01619969), Balapiravir (NCT01096576), and UV-4B(NCT02061358). NCT02696291) has entered the clinical stage.
The development of novel DENV inhibitors remains urgent. Over the past five years, antiviral inhibitors have been designed to target essential proteins and host factors in the dengue virus life cycle. The targets include NS3/NS2B protease, NS3 helicase E protein, and NS5 RNA-dependent RNA polymerase (RdRp).
NS3/2B Protease Inhibitors
NS3/2Bpro inhibitors need to compete with substrate peptides with P1 and P2 positions, which are essential Arg responses. α-Ketoamide and tri/tetrapeptide (three or four are found to contain the remaining peptide containing an electrophilic group to interact with the catalytic pocket. NS2B/NS3-IN-2 is a potent covalent inhibitor of dengue virus NS2B/NS3 with an IC50 of 6.0 nM, NS2B/NS3-IN-2 is non-cytotoxic and significantly improves cell viability. DV-B-120 is a competitive inhibitor of dengue virus (DENV), inhibits DENV-1, DENV-2, DENV-3 and DENV-4 with IC50 of 5.35, 7.39, 10.49 and 8.58 μM by inhibiting the NS2B-NS3 protease.
NS3 helicase inhibitors
The benzoxazole inhibitor ST-610 is reported by Byrd, which is a potent inhibitor of DE NV2 (EC50=0.272 μM). The compound is non-toxic to DENV1-4 in cell culture and is mutagenic in the Ames assay. The A263T mutation mapped on a basic patch within the NS3heli channel correlates with susceptibility to ST-610. Another report by Basavannacharya et al. A method for the analysis of NS3heli molecular beacon helicase was constructed. By screening a library of 1600 compounds, they determined that Surumin was a potent, noncompetitive inhibitor.
RdRp inhibitors
In order to inhibit the DENV virus RdRp, several methods have been introduced: nucleosides or their analogues that terminate RNA replication. Non-nucleosides that block allosteric sites and affect RdRp activity (e.g., N-sulfonylanthraceneamide derivatives, sofosbuvir, and HeE1-2Tyr, 66E2) and metal chelators (DMB220) that target essential ions in the catalytic process.
Inhibitors that target other viral proteins
A team of researchers from Novartis reported the activity of spiropyrrolopyridone against NS4B. The first is a racemate screened from DENV2 replicon analysis. After separating the enantiomers, they found compounds with better activity in the R enantiomers (1a). Compound 1a inhibits DENV2 and DENV3, but does not have the same effect on DENV1 and DENV4.
References
- Kuhn, Richard J., et al., Structure of dengue virus: implications for flavivirus organization, maturation, and fusion. Cell 108.5 (2002): 717-725.
- Sinha, Saumya, et al., Dengue virus pathogenesis and host molecular machineries. Journal of Biomedical Science 31.1 (2024): 43.
- Martina, Byron EE, et al., Dengue virus pathogenesis: an integrated view. Clinical microbiology reviews 22.4 (2009): 564-581.
- Tian, Yu-Shi, et al., Dengue virus and its inhibitors: a brief review. Chemical and Pharmaceutical Bulletin 66.3 (2018): 191-206.
- Siritt, Maria Eugenia Guzman, et al., Dengue: a continuing global threat. Nature Reviews Microbiology 8.12 (2010): S7-S16.
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