612-42-0

Basic information

• Product Name: N-(2-CARBOXYPHENYL)GLYCINE
• Synonyms: 2-(CARBOXYMETHYL-AMINO)-BENZOIC ACID;AKOS AU36-M366;AKOS BBS-00007771;TIMTEC-BB SBB006542;N-(2-CARBOXYPHENYL)GLYCINE;N-PHENYLGLYCINE-O-CARBOXYLIC ACID;N-(CARBOXYPHENYL)GLYCINE;N-(CARBOXYMETHYL)ANTHRANILIC ACID
• CAS NO: 612-42-0
• Molecular Formula: C₉H₉NO₄
• Molecular Weight: 195.17
• EINECS: 210-311-5
• Product Categories: Miscellaneous;Glycine Derivatives;Peptide Synthesis;Unnatural Amino Acid Derivatives
• Mol File: 612-42-0.mol
• Article Data: 21

Chemical Properties

• Melting Point: 218 °C (dec.)(lit.)
• Boiling Point: 218°C
• Flash Point: 218°C/
• Appearance: Light yellow to yellow/Crystalline Powder
• Density: 1.472
• Vapor Pressure: 3.31E-10mmHg at 25°C
• Refractive Index: 1.5700 (estimate)
• Storage Temp.: Sealed in dry,Room Temperature
• PKA: 3?+-.0.36(Predicted)
• CAS DataBase Reference: N-(2-CARBOXYPHENYL)GLYCINE(CAS DataBase Reference)
• NIST Chemistry Reference: N-(2-CARBOXYPHENYL)GLYCINE(612-42-0)
• EPA Substance Registry System: N-(2-CARBOXYPHENYL)GLYCINE(612-42-0)

Safety Data

• Hazard Codes: Xi
• Statements: 36/37/38
• Safety Statements: 26-37/39
• WGK Germany: 3
• TSCA: Yes
• HazardClass: IRRITANT
• Hazardous Substances Data: 612-42-0(Hazardous Substances Data)

Usage

Purification Methods

Crystallise the acid from hot water (charcoal). It forms complexes with Cu2+, Zn2+, Cd2+, Co2+ and Ni2+ in aqueous dioxane. [Roileanu et al. Rev Roum Chim 12 105 1967, Aldrich library of 13C, 1H FTNMR Spectra, NMR 2 1181A, Beilstein 14 H 348, 14 I 544, 14 II 225, 14 III 938.]

InChI:InChI=1/C9H9NO4/c11-8(12)5-10-7-4-2-1-3-6(7)9(13)14/h1-4,10H,5H2,(H,11,12)(H,13,14)

Upstream product

• 121163-57-3 N-carboxymethyl-N-nitroso-anthranilic acid 
• 23354-00-9 oxamide-N,N'-diacetic acid 
• 118-91-2 ortho-chlorobenzoic acid 
• 7732-18-5 water 
• 118-92-3 anthranilic acid 
• 79-11-8 chloroacetic acid 
• 56-81-5 glycerol 
• 7647-01-0 hydrogenchloride 
• 25784-02-5 2-(carbamoylmethylamino)benzoic acid 
• 50794-23-5 o-formylphenylglycine 
• 105528-49-2 2-(carboxymethyl-amino)-4-sulfo-benzoic acid 
• 56424-79-4 N-carbamoylmethyl-anthranilic acid methyl ester 
• 3926-62-3 sodium monochloroacetic acid 
• 552-37-4 sodium o-aminobenzoate 

Downstream Products

• 120-72-9 indole 
• 608-08-2 3-indoxyl acetate 
• 32253-75-1 5-bromo-2-<(carboxymethyl)amino>-benzoic acid 
• 861608-81-3 3,5-dibromo-2-(carboxymethyl-amino)-benzoic acid 
• 16851-69-7 2-(N-(carboxymethyl)acetamido)benzoic acid 
• 26490-97-1 2-Carboxy-4-iodophenylglycine 
• 480-93-3 indoxyl 
• 101724-29-2 2-Carboxy-4,6-dichlorophenylglycine 
• 133433-34-8 5-chloro-2-<(carboxymethyl)amino>-benzoic acid 
• 121163-57-3 N-carboxymethyl-N-nitroso-anthranilic acid 
• 482-89-3 1H,1H'-2,2'-Biindolylidene-3,3'-dione 
• 5933-35-7 N-(2-nitrophenyl)anthranilic acid 
• 75835-28-8 anhydro-5-acetoxy-2-hydroxyoxazolo<3,2-a>quinolinium hydroxide 
• 99692-18-9 C₁₅H₂₅NO₄Si₂ 

Relevant articles and documents

Indirubin Derivatives as Dual Inhibitors Targeting Cyclin-Dependent Kinase and Histone Deacetylase for Treating Cancer

To utilize the unique scaffold of a natural product indirubin, we herein adopted the strategy of combined pharmacophores to design and synthesize a series of novel indirubin derivatives as dual inhibitors against cyclin-dependent kinase (CDK) and histone deacetylase (HDAC). Among them, the lead compound 8b with remarkable CDK2/4/6 and HDAC6 inhibitory activity of IC50 = 60.9 ± 2.9, 276 ± 22.3, 27.2 ± 4.2, and 128.6 ± 0.4 nM, respectively, can efficiently induce apoptosis and S-phase arrest in several cancer cell lines. In particular, compound 8b can prevent the proliferation of a non-small-cell lung cancer cell line (A549) through the Mcl-1/XIAP/PARP axis, in agreement with the unique modes of action of the combined agents of HDAC inhibitors and CDK inhibitors. In an A549 xerograph model, compound 8b showed significant antitumor efficacy correlated with its dual inhibition. Our data demonstrated that compound 8b as a single agent could be a promising drug candidate for cancer therapy in combination with CDK and HDAC inhibitors.

Synthesis and biological evaluation of indoloquinoline alkaloid cryptolepine and its bromo-derivative as dual cholinesterase inhibitors

Alkaloids have always been a great source of cholinesterase inhibitors. Numerous studies have shown that inhibiting acetylcholinesterase as well as butyrylcholinetserase is advantageous, and have better chances of success in preclinical/ clinical settings. With the objective to discover dual cholinesterase inhibitors, herein we report synthesis and biological evaluation of indoloquinoline alkaloid cryptolepine (1) and its bromo-derivative 2. Our study has shown that cryptolepine (1) and its 2-bromo-derivative 2 are dual inhibitors of acetylcholinesterase and butyrylcholinesterase, the enzymes which are involved in blocking the process of neurotransmission. Cryptolepine inhibits Electrophorus electricus acetylcholinesterase, recombinant human acetylcholinesterase and equine serum butyrylcholinesterase with IC50 values of 267, 485 and 699 nM, respectively. The 2-bromo-derivative of cryptolepine also showed inhibition of these enzymes, with IC50 values of 415, 868 and 770 nM, respectively. The kinetic studies revealed that cryptolepine inhibits human acetylcholinesterase in a non-competitive manner, with ki value of 0.88 μM. Additionally, these alkaloids were also tested against two other important pathological events of Alzheimer's disease viz. stopping the formation of toxic amyloid-β oligomers (via inhibition of BACE-1), and increasing the amyloid-β clearance (via P-gp induction). Cryptolepine displayed potent P-gp induction activity at 100 nM, in P-gp overexpressing adenocarcinoma LS-180 cells and excellent toxicity window in LS-180 as well as in human neuroblastoma SH-SY5Y cell line. The molecular modeling studies with AChE and BChE have shown that both alkaloids were tightly packed inside the active site gorge (site 1) via multiple π-π and cation-π interactions. Both inhibitors have shown interaction with the allosteric “peripheral anionic site” via hydrophobic interactions. The ADME properties including the BBB permeability were computed for these alkaloids, and were found within the acceptable range.

Orally Effective Aminoalkyl 10H-Indolo[3,2-b]quinoline-11-carboxamide Kills the Malaria Parasite by Inhibiting Host Hemoglobin Uptake

A series of indolo[3,2-b]quinoline-C11-carboxamides were synthesized by incorporation of aminoalkyl side chains into the core of indolo[3,2-b]quinoline-C11-carboxylic acid. Their in vitro antiplasmodial evaluation against Plasmodium falciparum led to the identification of a 2-(piperidin-1-yl)ethanamine-linked analogue {2-bromo-N-[2-(piperidin-1-yl)ethyl]-10H-indolo[3,2-b]quinoline-11-carboxamide (3 g)} (IC50=1.3 μm) as the most promising compound exhibiting good selectivity indices against mammalian cell lines. The kill kinetics on erythrocytic-stage parasites revealed that 3 g caused complete killing of only the trophozoite-stage parasites. Mechanistic studies showed that 3 g targets the food vacuole of the parasite and inhibits hemoglobin uptake, β-hematin formation, and the basic endocytic processes of the parasite. Analogue 3 g was found to be orally bioavailable, and its curative antimalarial studies at 50 mg per kg p.o. against a Plasmodium berghei (ANKA)-infected mouse model revealed that mice treated with 3 g showed 27–35 % suppression of parasitemia with an increase in life span relative to untreated, control mice. Thus, the present work demonstrated a proof of concept for the oral efficacy of indolo[3,2-b]quinoline-C11-carboxamides.