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γ-[4-(p-Chloro-α-hydroxybenzyl)piperidino]-p-fluorobutyrophenone, also known as 4-(p-chlorobenzyl)-1-(4-fluorophenyl)-4-piperidinol, is a complex organic compound with the molecular formula C22H24ClFNO2. It is a derivative of butyrophenone, a class of drugs that act as dopamine antagonists, and is characterized by the presence of a chlorinated benzyl group attached to a piperidine ring and a fluorinated butyrophenone core. This chemical has been studied for its potential psychoactive effects and is often associated with research chemicals due to its structural similarity to known psychoactive substances. It is important to note that the synthesis, distribution, and use of such compounds may be subject to legal restrictions and regulations depending on the jurisdiction.

38077-13-3

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38077-13-3 Usage

Check Digit Verification of cas no

The CAS Registry Mumber 38077-13-3 includes 8 digits separated into 3 groups by hyphens. The first part of the number,starting from the left, has 5 digits, 3,8,0,7 and 7 respectively; the second part has 2 digits, 1 and 3 respectively.
Calculate Digit Verification of CAS Registry Number 38077-13:
(7*3)+(6*8)+(5*0)+(4*7)+(3*7)+(2*1)+(1*3)=123
123 % 10 = 3
So 38077-13-3 is a valid CAS Registry Number.

38077-13-3Downstream Products

38077-13-3Relevant academic research and scientific papers

Design, Synthesis, and Evaluation of Metabolism-Based Analogues of Haloperidol Incapable of Forming MPP+-like Species

Lyles-Eggleston,Altundas,Xia,Sikazwe,Fan,Yang,Li,Zhang,Zhu,Schmidt,Vanase-Frawley,Shrihkande,Villalobos,Borne,Ablordeppey

, p. 497 - 508 (2007/10/03)

The long-term, irreversible, Parkinsonism-like side effects of haloperidol have been speculated to involve several mechanisms. More recently, it has been speculated that the metabolic transformation to MPP+-like species may contribute to the Parkinsonism-like side effects. Because BCPP+ and its reduced analogue have been shown to possess the potential to destroy dopamine receptors in the nigrostriatum, we have designed new analogues of haloperidol lacking the structural features necessary to form neurotoxic quaternary species but retaining their dopamine-binding capacity. The most potent agent at the D2 receptor, the homopiperidine analogue 11, was found to be equipotent to haloperidol. It was also of interest to identify analogues with DA binding profiles similar to that of clozapine at the dopamine receptor subtypes. Evaluation of the proposed agents shows that the ratio of D2 to D4 (2) binding of clozapine was mimicked by 7 [Ki(D2) = 33, Ki(D3) = 200, Ki(D4) = 11 nM; Ki(D2)/Ki(D4) = 3] and 9 [Ki(D2) = 44, Ki(D3) = 170, Ki(D4) = 24 nM; Ki(D2)/Ki(D4) = 2]. A preliminary in-vivo testing of compound 7 shows that its behavioral profile is similar to that of clozapine. This profile suggests that there is a need for further evaluation of these two synthetic agents and their enantiomers for efficacy and lack of catalepsy in animal models.

Method for inhibiting emesis and compositions therefor

-

, (2008/06/13)

1,4-(3-)Disubstituted piperidines are disclosed which have useful antiemetic properties. The compounds have the general formula: STR1 wherein R is halogen, R1 is hydrogen and halogen, n is a positive integer from 2-4 and A is --C(O)-- and --CHO

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