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1-(4-chlorobenzyl)piperidin-3-ol is a chemical with a specific purpose. Lookchem provides you with multiple data and supplier information of this chemical.

408312-64-1

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408312-64-1 Usage

Chemical structure

Piperidine derivative with a hydroxyl group attached to the third carbon of the piperidine ring and a 4-chlorobenzyl group at the first carbon.

Pharmaceutical use

Building block for the synthesis of various drugs and drug candidates.

Potential applications

Central nervous system depressant, analgesic, treatment of pain, and neurological disorders.

Physical appearance

White to off-white crystalline powder.

Solubility

Soluble in organic solvents, low solubility in water.

Ongoing research

Exact biological and pharmacological effects are still being investigated.

Check Digit Verification of cas no

The CAS Registry Mumber 408312-64-1 includes 9 digits separated into 3 groups by hyphens. The first part of the number,starting from the left, has 6 digits, 4,0,8,3,1 and 2 respectively; the second part has 2 digits, 6 and 4 respectively.
Calculate Digit Verification of CAS Registry Number 408312-64:
(8*4)+(7*0)+(6*8)+(5*3)+(4*1)+(3*2)+(2*6)+(1*4)=121
121 % 10 = 1
So 408312-64-1 is a valid CAS Registry Number.

408312-64-1Downstream Products

408312-64-1Relevant academic research and scientific papers

Design and synthesis of Rho kinase inhibitors (II)

Iwakubo, Masayuki,Takami, Atsuya,Okada, Yuji,Kawata, Takehisa,Tagami, Yoshimichi,Ohashi, Hiroshi,Sato, Motoko,Sugiyama, Terumi,Fukushima, Kayoko,Iijima, Hiroshi

, p. 350 - 364 (2008/02/04)

In a previous study, we identified several structurally unrelated scaffolds of the Rho kinase inhibitor using pharmacophore information obtained from the results of a high-throughput screening and structural information from a homology model of Rho kinase. 1H-Indazole is one of the candidate scaffolds on which a new series of potent Rho kinase inhibitors could be developed. In this study, the detailed structure-activity relationship of 1H-indazole analogues was studied. During this study, we found that the cell-free enzyme inhibitory potential of Rho kinase inhibitors having the 1H-indazole scaffold did not necessarily correlate with their inhibitory potential toward the chemotaxis of cultured cells. The choice of the linker substructure was shown to be an important factor for the 1H-indazole analogues to inhibit the chemotaxis of cells. Optimization of the 1H-indazole inhibitors with respect to the in vitro inhibition of monocyte chemotaxis induced by MCP-1 was carried out. The inhibitory potential was improved both in the cell-free enzyme assay and in the chemotaxis assay.

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