Design and Synthesis of Pyrrolidine-5,5-<i>trans-</i>lactams (5-Oxohexahydropyrrolo[3,2-<i>b</i>]pyrroles) as Novel Mechanism-Based Inhibitors of Human Cytomegalovirus Protease. 2. Potency and Chirality

Borthwick, Alan D.; Crame, Andrew J.; Ertl, Peter; Exall, Anne M.; Haley, Terry; Hart, Graham; Mason, Andrew M.; Pennell, Andrew M. K.; Singh, Onkar; Weingarten, Gordon G.; Woolven, James M.

doi:10.1021/jm0102203

Cited by 63 publications

(45 citation statements)

References 17 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…77,79 Sulfonamide-based antivirals were also recently designed against the HCMV protease. 80 In contrast to the HIV PR discussed earlier, this enzyme belongs to the serine PR family, and together with similar proteases isolated from other herpes viruses, it is characterized by a particular catalytic triad, of the type His, His, Ser within the active site. 81 It was observed that a-methylpyrrolidine-5,5-trans-lactam derivatives of type 80 act as mechanism-based inhibitors of the HCMV dAla protease, acylating reversibly and in a timedependent manner the active site nucleophile Ser 132.…”

Section: H E R P E S V I R U S E S ( H S V a N D H C M V ) P R O T mentioning

confidence: 96%

“…Compounds of type 82 bind to this PR with the 6-Me group within the S 1 subsite, the N-4-cyclopropylcarbonyl moiety within the S 1 0 subsite and the bulky, hydrophobic arylsulfonylpyrrolidine-2-carbonyl moiety within the S 3 subsite. 80 Derivatives incorporating the dansyl-(S)-proline moiety in this position showed the best activity (IC 50 of 0.34 mM) and also specificity over related serine proteases (such as elastase, thrombin, or acetyl cholinesterase), which were inhibited with IC 50 values in the range of 10-200 mM.…”

Section: H E R P E S V I R U S E S ( H S V a N D H C M V ) P R O T mentioning

confidence: 96%

“…81 It was observed that a-methylpyrrolidine-5,5-trans-lactam derivatives of type 80 act as mechanism-based inhibitors of the HCMV dAla protease, acylating reversibly and in a timedependent manner the active site nucleophile Ser 132. 80 This serine PR hydrolyzes peptide bonds of the type Ala-Ser. Compounds of type 82 bind to this PR with the 6-Me group within the S 1 subsite, the N-4-cyclopropylcarbonyl moiety within the S 1 0 subsite and the bulky, hydrophobic arylsulfonylpyrrolidine-2-carbonyl moiety within the S 3 subsite.…”

Section: H E R P E S V I R U S E S ( H S V a N D H C M V ) P R O T mentioning

confidence: 99%

See 2 more Smart Citations

Protease inhibitors of the sulfonamide type: Anticancer, antiinflammatory, and antiviral agents

Supuran

Casini

Scozzafava

2003

Medicinal Research Reviews

393

153

View full text Add to dashboard Cite

The sulfonamides constitute an important class of drugs, with several types of pharmacological agents possessing antibacterial, anticarbonic anhydrase, diuretic, hypoglycemic, and antithyroid activity among others. A large number of structurally novel sulfonamide derivatives have ultimately been reported to show substantial protease inhibitory properties. Of particular interest are some metalloprotease inhibitors belonging to this class, which by inhibiting several matrix metalloproteases (MMPs) show interesting antitumor properties. Some of these compounds are currently being evaluated in clinical trials. The large number of sulfonamide MMP inhibitors ultimately reported also lead to the design of effective tumor necrosis factor-alpha converting enzyme (TACE) inhibitors, potentially useful in the treatment of inflammatory states of various types. Since both MMPs and TACE contribute synergistically to the pathophysiology of many diseases, such as arthritis, bacterial meningitis, tumor invasion; the dual inhibition of these enzymes emerged as an interesting target for the drug design of anticancer/antiinflammatory drugs, and many such sulfonamide derivatives were recently reported. Human neutrophyl elastase (HNE) inhibitors of the sulfonamide type may also be useful in the treatment of inflammatory conditions, such as emphysema, cystic fibrosis, chronic bronchitis, ischemia reperfusion injury, and acute respiratory distress syndrome. Inhibition of some cysteine proteases, such as several caspase and cathepsin isozymes, may lead to the development of pharmacological agents effective for the management of several diseases, such as rheumatoid arthritis, inflammatory bowel disease, brain damage, and stroke. Another research line that progressed much in the last time regards different sulfonamides with remarkable antiviral activity. Some clinically used HIV protease inhibitors (such as amprenavir) possess sulfonamide moieties in their molecules, which are critical for the potency of these drugs, as shown by means of X-ray crystallography, whereas a very large number of other derivatives are constantly being synthesized and evaluated in order to obtain compounds with lower toxicity or augmented activity against viruses resistant to the such first generation drugs. Other viral proteases, such as those isolated from several types of herpes viruses may be inhibited by sulfonamide derivatives, leading thus to more effective classes of antiviral drugs.

show abstract

Section: H E R P E S V I R U S E S ( H S V a N D H C M V ) P R O T mentioning

confidence: 96%

Section: H E R P E S V I R U S E S ( H S V a N D H C M V ) P R O T mentioning

confidence: 96%

Section: H E R P E S V I R U S E S ( H S V a N D H C M V ) P R O T mentioning

confidence: 99%

See 1 more Smart Citation

Protease inhibitors of the sulfonamide type: Anticancer, antiinflammatory, and antiviral agents

Supuran

Casini

Scozzafava

2003

Medicinal Research Reviews

393

153

View full text Add to dashboard Cite

show abstract

“…We ultimately focused on two types of functionalization: acylation (including phosphonylation and sulfonylation) and arylation. Additional possible N-functionalization reactions of a related bicyclic substrate have been summarized in the work of Borthwick et al (33).…”

mentioning

confidence: 99%

Ammonia synthons for the multicomponent assembly of complex γ-lactams

Tan

Martin

Fettinger

et al. 2011

Proc. Natl. Acad. Sci. U.S.A.

View full text Add to dashboard Cite

The synthesis of γ-lactams that are unsubstituted at the 1-position (nitrogen) as well as their subsequent N -functionalization is reported. A recently discovered four-component reaction (4CR) is employed with either an ammonia precursor or a protected form of ammonia that can be deprotected in a subsequent synthetic step. These methods represent the first multicomponent assembly of complex lactam structures that are unsubstituted at nitrogen. In addition, two methods for the introduction of nitrogen substituents that are not possible through the original 4CR are reported. X-ray crystallographic analysis of representative structures reveals conformational changes in the core structure that will enable future deployment of this chemistry in the design and synthesis of diverse collections of lactams suitable for the discovery of new biological probes.

show abstract

“…Organic compounds containing nitrogenheterocyclic rings are important compounds in medicinal chemistry. Recently, because of their specially pharmaceutical and biological activities, compounds with pyrrole rings such as dihydro-2-oxypyrroles and Biginelli [5] reactions for the synthesis of 3, 4-dihydropyrimidin-2-(1H)-ones derivatives have attracted much interest in the organic researches for example these compounds have been used as anticancer [6], calcium channel blockers, α-1a-antagonists [7], human cytomegalovirus ( HCMV) protease [8], they has been used as Pl-091 [9], many of number alkaloids with biological activities have pyrrole rings [10], And these rings have been used as UCS1025A [11]. In the recent years, several protocols for the preparation of these compounds that is including bronsted or lewis acid catalysts have been reported for example Cu(OAc) 2 [12], [Btto][p-TSA] [13], bakers , yeast [14], Calcium Fluoride [15], copper(II) tetrafluoroborate [16], hydrotalcite [17], TBAB [18], hexaaquaaluminium(III) tetrafluoroborate [19], copper(II)sulfamate [20], I 2 [21], AcOH [22], [n-Bu 4 3 [24], oxalic acid [25], ZrCl 4 [26], InCl 3 [27].…”

Section: Introductionmentioning

confidence: 99%

Phthalic Acid: A Green, Biodegradable and Environmentally Benign Nature Di-Functional Brønsted Acid Catalyst for the One-Pot Synthesis of 3, 4-Dihydropyrimidin-2- (1h)-One Derivatives and Substituted Dihydro-2-Oxypyrroles

Mohamadpour

Lashkari

Maghsoodlou

et al. 2018

J. Chil. Chem. Soc.

View full text Add to dashboard Cite

Phthalic acid as a green, biodegradable economical and environmentally benign nature catalyst for the one-pot three-component Biginelli synthesis of 3,4-dihydropyrimidin-2-(1H)-one derivatives via β-keto esters, aldehyde derivatives and urea/thiourea under thermal and solvent-free conditions and one-pot four-component domino condensation of substituted dihydro-2-oxypyrrole by reaction of dialkyl acetylenedicarboxylate, formaldehyde and amines (aromatic and aliphatic) under ambient temperature with short reaction times and excellent yields is reported. The most benefits this procedure are such as green, biodegradable, inexpensive and non-toxic catalyst, eco-friendly, high catalytic activity, efficient, easily separation with no column chromatographic separation, simple operational procedures, one-pot, excellent yields, environmentally benign nature.

show abstract

Design and Synthesis of Pyrrolidine-5,5-trans-lactams (5-Oxohexahydropyrrolo[3,2-b]pyrroles) as Novel Mechanism-Based Inhibitors of Human Cytomegalovirus Protease. 2. Potency and Chirality

Cited by 63 publications

References 17 publications

Protease inhibitors of the sulfonamide type: Anticancer, antiinflammatory, and antiviral agents

Protease inhibitors of the sulfonamide type: Anticancer, antiinflammatory, and antiviral agents

Ammonia synthons for the multicomponent assembly of complex γ-lactams

Phthalic Acid: A Green, Biodegradable and Environmentally Benign Nature Di-Functional Brønsted Acid Catalyst for the One-Pot Synthesis of 3, 4-Dihydropyrimidin-2- (1h)-One Derivatives and Substituted Dihydro-2-Oxypyrroles

Contact Info

Product

Resources

About