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84693-92-5

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84693-92-5 Usage

Check Digit Verification of cas no

The CAS Registry Mumber 84693-92-5 includes 8 digits separated into 3 groups by hyphens. The first part of the number,starting from the left, has 5 digits, 8,4,6,9 and 3 respectively; the second part has 2 digits, 9 and 2 respectively.
Calculate Digit Verification of CAS Registry Number 84693-92:
(7*8)+(6*4)+(5*6)+(4*9)+(3*3)+(2*9)+(1*2)=175
175 % 10 = 5
So 84693-92-5 is a valid CAS Registry Number.
InChI:InChI=1/C18H23FO2/c1-18-7-6-13-12-5-3-11(20)8-10(12)2-4-14(13)15(18)9-16(19)17(18)21/h3,5,8,13-17,20-21H,2,4,6-7,9H2,1H3/t13-,14-,15+,16+,17+,18+/m1/s1

84693-92-5Downstream Products

84693-92-5Relevant articles and documents

16β-(Fluoro)estrogens: Systematic Investigation of a New Series of Fluorine-18-Labeled Estrogens as Potential Imaging Agents for Estrogen-Receptor-Positive Breast Tumors

VanBrocklin, Henry F.,Carlson, Kathryn E.,Katzenellenbogen, John A.,Welch, Michael J.

, p. 1619 - 1629 (1993)

In order to understand the structural features that might lead to an estrogen receptor (ER) based breast tumor imaging agent with improved uptake characteristics, we have synthesized several new analogs of 16β-fluoroestradiol (βFES) and studied their tissue distribution in immature rats. The compounds we prepared were 11β-methoxy-βFES (7a), 11β-ethyl-βFES (7b), 17α-ethynyl-βFES (8c), 17α-ethynyl-11β-methoxy-βFES (8a), and 11β-ethyl-17α-ethynyl-βFES (8b). All of the analogs exhibit good affinity for ER, ranging at 25 deg C from 10 to 460, with estradiol equal to 100. Measurement of their octanol/water partition coefficients by an HPLC method allowed us to estimate their level of nonspecific binding and thereby to predict their binding selectivity indices (BSI, i.e., the ratio of their ER-specific to nonspecific binding); the BSI values of three fluorine-substituted analogs exceed that of estradiol. These ligands have been labeled in the 16β position with fluorine-18 by the nucleophilic displacement of an α-disposed trifluoromethanesulfonate by fluoride ion. Reduction with lithium aluminum hydride produced the estradiol series (-7a-c), while treatment with lithium trimethylsilylacetylide afforded the ethynylated series (-8a-c). The synthesis time was 85 min for -7a-c and 120 min for -8a-c, with radiochemical yields ranging from 16 to 43percent, and effective specific activities being 90-2900 Ci/mmol (3.3-107 TBq/mmol). In tissue distribution studies in immature female rats, all of the labeled analogs demonstrated ER-selective uptake in the principal target tissues, the uterus and the ovaries, and also in organs with lower titers of ER, the secondary target sites kidney, thymus, fat, and muscle. Although factors other than specific and nonspecific binding obviously affect the tissue distribution of these 16β-fluoroestrogens, we find that their ER-specific uptake by both the principal and the secondary target tissues correlates with their BSI values at a high level of statistical significance in most cases. The ethynylated-11β-methoxy analog -8a had high selectivity (uterus to blood ratio) after 3 h and exhibited the highest uterine uptake (percent injected dose/gram) of any fluorine-substituted estradiol ligand we have studied to date. This compound has been chosen for more detailed studies (to be described elsewhere), including clinical trials in human patients diagnosed with primary breast cancer.

Synthesis of 16-fluoroestrogens by unusually facile fluoride ion displacement reactions: Prospects for the preparation of fluorine-18 labeled estrogens

Kiesewetter,Katzenellenbogen,Kilbourn,Welch

, p. 4900 - 4905 (2007/10/02)

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