연구용
제품 번호: S8133
| 세포주 | 분석 유형 | 농도 | 배양 시간 | 제형 | 활성 설명 | PMID |
|---|---|---|---|---|---|---|
| PBMC | Function assay | 30 nM | 18 hrs | Induction of type 1 IFN secretion in human PBMC at 30 nM after 18 hrs by ELISA, Activity=0.00125μM. | 20232824 | |
| PBMC | Function assay | 10 nM | 18 hrs | Induction of type 1 IFN secretion in human PBMC at 10 nM after 18 hrs by ELISA, Activity<0.00125μM. | 20232824 | |
| PBMC | Function assay | 100 nM | 18 hrs | Induction of type 1 IFN secretion in human PBMC at 100 nM after 18 hrs by ELISA, Activity=0.00561μM. | 20232824 | |
| PBMC | Function assay | 300 nM | 18 hrs | Induction of type 1 IFN secretion in human PBMC at 300 nM after 18 hrs by ELISA, Activity=0.00726μM. | 20232824 | |
| PBMC | Function assay | 1000 nM | 18 hrs | Induction of type 1 IFN secretion in human PBMC at 1000 nM after 18 hrs by ELISA, Activity=0.00775μM. | 20232824 | |
| Huh7 | Antiviral assay | 48 hrs | Antiviral activity against HCV infected human Huh7 replicon cells treated for 48 hrs with drug-induced mixed donor human PBMC supernatants assessed as viral levels by luciferase assay, EC50=0.024μM. | 17548497 | ||
| Huh7 | Antiviral assay | 48 hrs | Antiviral activity against HCV infected human Huh7 replicon cells treated for 48 hrs with drug-induced single donor human PBMC supernatants assessed as viral levels by luciferase assay, EC50=0.0265μM. | 17548497 | ||
| PBMC | Function assay | 24 hrs | Induction of IFNalpha2a level in human PBMC assessed as drug level causing maximal cytokine induction after 24 hrs relative to control, Activity=0.1μM. | 17548497 | ||
| PBMC | Function assay | 24 hrs | Toxic induction of IL1-beta level in human PBMC assessed as drug level causing maximal cytokine induction after 24 hrs relative to control, Activity=1μM. | 17548497 | ||
| PBMC | Function assay | 24 hrs | Toxic induction of IL6 level in human PBMC assessed as drug level causing maximal cytokine induction after 24 hrs relative to control, Activity=1μM. | 17548497 | ||
| PBMC | Function assay | 24 hrs | Toxic induction of TNFalpha level in human PBMC assessed as drug level causing maximal cytokine induction after 24 hrs relative to control, Activity=1μM. | 17548497 | ||
| HEK293 | Function assay | 6 hrs | Agonist activity at human TLR7 expressed in HEK293 cells after 6 hrs by NFkappaB-luciferase reporter gene assay, MEC=0.1μM. | 30143425 | ||
| HEK293 | Function assay | Agonist activity at human TLR7 expressed in HEK293 cells coexpressing pNiFty2-SEAP reporter by reporter gene assay, EC50=0.2601μM. | 20232824 | |||
| HEK293 | Function assay | 6 hrs | Agonist activity at human TLR8 expressed in HEK293 cells after 6 hrs by NFkappaB-luciferase reporter gene assay, MEC=0.3μM. | 30143425 | ||
| HEK | Function assay | 8 to 12 hrs | Agonist activity at human TLR7 expressed in HEK cells after 8 to 12 hrs by NFkappaB/SEAP reporter gene assay, EC50=1.34μM. | 29152046 | ||
| HEK | Function assay | 24 hrs | Agonist activity at human TLR7 transfected in HEK cells assessed as NFkappaB induction after 24 hrs by specific secreted alkaline phosphatase gene assay, EC50=1.4μM. | 22837811 | ||
| HEK293 | Function assay | 24 hrs | Agonist activity at human TLR-7 expressed in HEK293 cells after 24 hrs by SEAP reporter gene assay, EC50=1.5μM. | 24383475 | ||
| HEK293 | Function assay | 6 hrs | Agonist activity at human TLR8 expressed in HEK293 cells incubated for 6 hrs by luciferase reporter gene assay, EC50=4μM. | 27270029 | ||
| HEK293 | Function assay | 24 hrs | Agonist activity at human TLR-8 expressed in HEK293 cells after 24 hrs by SEAP reporter gene assay, EC50=4.5μM. | 24383475 | ||
| HEK | Function assay | 8 to 12 hrs | Agonist activity at human TLR8 expressed in HEK cells after 8 to 12 hrs by NFkappaB/SEAP reporter gene assay, EC50=6.13μM. | 29152046 | ||
| HEK | Function assay | 24 hrs | Agonist activity at human TLR8 transfected in HEK cells assessed as NFkappaB induction after 24 hrs by specific secreted alkaline phosphatase gene assay, EC50=6.4μM. | 22837811 | ||
| PBMC | Function assay | 24 hrs | Increase in IFNalpha level in human PBMC after 24 hrs relative to control | 17548497 | ||
| PBMC | Function assay | 24 hrs | Increase in 2',5'-oligoadenylate synthase level in human PBMC after 24 hrs relative to control | 17548497 | ||
| PBMC | Toxicity assay | 24 hrs | Toxicity assessed as increase in IL6 level in human PBMC after 24 hrs relative to control | 17548497 | ||
| Huh7 | Antiviral assay | 24 hrs | Antiviral activity against HCV infected human Huh7 replicon cells treated for 24 hrs with drug-induced human PBMC supernatants assessed as viral levels by luciferase assay | 17548497 | ||
| Huh7 | Antiviral assay | Antiviral activity against HCV infected human Huh7 replicon cells treated with drug-induced human PBMC supernatants assessed as viral levels by luciferase assay | 17548497 | |||
| PBMC | Function assay | 22.5 uM | 24 hrs | Agonist activity at TLR7/TLR8 in human PBMC assessed as induction of TNF-alpha production at 22.5 uM after 24 hrs by flow cytometric analysis | 24383475 | |
| PBMC | Immunomodulatory assay | 16 uM | 24 hrs | Immunomodulatory activity in human PBMC assessed as induction of IL-6 secretion at 16 uM after 24 hrs by ELISA | 28254484 | |
| BMD | Function assay | 1 uM | 48 hrs | Induction of TLR7 receptor-mediated C57BL/6 mouse BMD cells activation assessed as upregulation of CD86 at 1 uM after 48 hrs by flow cytometry | 19299126 | |
| BMD | Function assay | 1 uM | 48 hrs | Induction of TLR7 receptor-mediated C57BL/6 mouse BMD cells activation assessed as upregulation of MHC class-2 at 1 uM after 48 hrs by flow cytometry | 19299126 | |
| BMD | Function assay | 1 uM | 48 hrs | Induction of TLR7 receptor-mediated C57BL/6 mouse BMD cells activation assessed as upregulation of CD40 at 1 uM after 48 hrs by flow cytometry | 19299126 | |
| BMD | Function assay | 5 uM | 24 hrs | Induction of TLR7 receptor-mediated C57BL/6 mouse BMD cells activation assessed as IL12 production at 5 uM after 24 hrs by ELISA | 19299126 | |
| 클릭하여 더 많은 세포주 실험 데이터 보기 | ||||||
| 분자량 | 314.38 | 화학식 | C17H22N4O2 |
보관 (수령일로부터) | |
|---|---|---|---|---|---|
| CAS 번호 | 144875-48-9 | SDF 다운로드 | 원액 보관 |
|
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| 동의어 | S28463 | Smiles | CCOCC1=NC2=C(N1CC(C)(C)O)C3=CC=CC=C3N=C2N | ||
|
In vitro |
DMSO
: 62 mg/mL
(197.21 mM)
Ethanol : 51 mg/mL Water : Insoluble |
|
In vivo |
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1단계: 아래 정보 입력 (권장: 실험 중 손실을 고려하여 추가 동물 포함)
2단계: 생체 내 제형 입력 (이것은 계산기일 뿐 제형이 아닙니다. 용해도 섹션에 생체 내 제형이 없는 경우 먼저 당사에 문의하십시오.)
계산 결과:
작업 농도: mg/ml;
DMSO 원액 준비 방법: mg 약물 사전 용해 μL DMSO ( 원액 농도 mg/mL, 농도가 해당 약물 배치의 DMSO 용해도를 초과하는 경우 먼저 당사에 문의하십시오. )
생체 내 제형 준비 방법: 취하다 μL DMSO 원액, 다음 추가μL PEG300, 혼합하고 투명하게 한 다음 추가μL Tween 80, 혼합하고 투명하게 한 다음 추가 μL ddH2O, 혼합하고 투명하게 합니다.
생체 내 제형 준비 방법: 취하다 μL DMSO 원액, 다음 추가 μL 옥수수 기름, 혼합하고 투명하게 합니다.
참고: 1. 다음 용매를 추가하기 전에 액체가 투명한지 확인하십시오.
2. 용매를 순서대로 추가해야 합니다. 다음 용매를 추가하기 전에 이전 추가에서 얻은 용액이 투명한 용액인지 확인해야 합니다. 와동, 초음파 또는 뜨거운 물 중탕과 같은 물리적 방법을 사용하여 용해를 도울 수 있습니다.
| Targets/IC50/Ki |
TLR7
TLR8
|
|---|---|
| 시험관 내(In vitro) |
Resiquimod (R-848) activates immune cells and induces proliferation of wild-type splenocytes via the Toll-like receptor 7 (TLR7)-MyD88-dependent signaling pathway. This compound also modulates dendritic cells to augment cytomegalovirus- and HIV-1-specific T cell responses. It induces the differentiation of myeloid-derived suppressor cells into macrophages and dendritic cells, and may improve cancer immunotherapy by reducing immunosuppressive MDSCs. |
| 생체 내(In vivo) |
In wild-type mice, Resiquimod (R-848) (50 nmol, i.p.) induces increased serum concentrations of IFN-alpha, TNF-alpha and IL-12, while neither TLR7-deficient mice nor MyD88-deficient mice show an increase in these cytokines. In a murine model of allergic asthma, this compound (i.n., 20 μg/mouse) reduces allergen induced airway reactivity and inflammation via reduction in Nrf2 signaling. |
참조 |
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(데이터 출처 https://clinicaltrials.gov, 업데이트 날짜 2024-05-22)
| NCT 번호 | 모집 | 조건 | 스폰서/협력자 | 시작일 | 단계 |
|---|---|---|---|---|---|
| NCT06021002 | Recruiting | Innate Inflammatory Response|Asthma|Nasal Allergy |
Cambridge University Hospitals NHS Foundation Trust |
August 9 2022 | Not Applicable |
| NCT04127864 | Active not recruiting | Colorectal Cancer|Surgery |
University of Copenhagen|Zealand University Hospital |
October 14 2019 | -- |
| NCT02688478 | Unknown status | Allergies |
University of British Columbia |
February 2 2017 | Not Applicable |
| NCT00960752 | Completed | Melanoma |
M.D. Anderson Cancer Center |
May 20 2010 | Phase 2 |