The chemistry and biology of guanidine natural products

Berlinck, Roberto G. S.; Bertonha, Ariane F.; Takaki, Mirelle; Rodríguez, Julie Paulin García

doi:10.1039/c7np00037e

Cited by 65 publications

(45 citation statements)

References 210 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…This strongly suggests that sulfo groups reduce PST toxi city, further highlighting their potential for incorporation into PSTbased drug candidates. The use of biosynthetic enzymes to modify PSTs represents a strategy that is distinct from the chemicalsynthesis approaches more frequently used to make analogues of these natural products 12 . Although many of those synthetic efforts have been successful, they often involve long sequences of reactions and deliver low yields of products as a con sequence of the challenging architectures of the PSTs -which contain an abundance of reactive oxygen and nitrogen atoms that com plicate the use of morestandard chemical reactions.…”

Section: Enzymes That Detoxify Marine Toxinsmentioning

confidence: 99%

Enzymes that detoxify marine toxins

McCallum¹,

Balskus²

2019

Nature

View full text Add to dashboard Cite

Section: Enzymes That Detoxify Marine Toxinsmentioning

confidence: 99%

Enzymes that detoxify marine toxins

McCallum¹,

Balskus²

2019

Nature

View full text Add to dashboard Cite

“…About one-third of all approved drugs classified as "small molecules" in this period are natural products, derived from natural or synthetic products but with a natural pharmacophore. Guanidine derivatives can be found in several natural products from diverse origin [9,10] and this structural unit is present as a building block in various pharmaceuticals such as rosuvastatin a cholesterol biosynthesis inhibitor, [11] guanabenz used clinically as an antihypertensive agent, [12] imatinib a tyrosine kinase inhibitor [13] used as an anticancer drug and the blockbuster drug used to treat peptic ulcers and cimetidine a histamine H2 receptor antagonist that inhibits stomach acid production [14]. Considered to be one of the strongest organic bases (pK HA = 13.6) guanidine has the capacity to bind to carboxylates, phosphates and metals with the guanidinium cation engaging special interactions between ligand/receptor or enzyme/substrate [15].…”

Section: Introductionmentioning

confidence: 99%

Synthetic Approaches to a Challenging and Unusual Structure—An Amino-Pyrrolidine Guanine Core

et al. 2020

View full text Add to dashboard Cite

The synthesis of an unreported 2-aminopyrrolidine-1-carboxamidine unit is here described for the first time. This unusual and promising structure was attained through the oxidative decarboxylation of amino acids using the pair of reagents, silver(I)/peroxydisulfate (Ag(I)/S2O82−) followed by intermolecular (in the case of l-proline derivative) and intramolecular trapping (in the case of acyl l-arginine) by N-nucleophiles. The l-proline approach has a broader scope for the synthesis of 2-aminopyrrolidine-1-carboxamidine derivatives, whereas the intramolecular cyclization afforded by the l-acylarginines, when applied, results in higher yields. The former allowed the first synthesis of cernumidine, a natural alkaloid isolated in 2011 from Solanum cernuum Vell, as its racemic form.

show abstract

“…It serves as a prominent functional group in essential metabolites including arginine, creatine, guanine, as well as in a wide range of secondary metabolites. 2 Due to its high pK a (13.6), it is a strong base and is positively charged under physiological conditions. Many of its applications are related to this unique property.…”

Section: Introductionmentioning

confidence: 99%