Novel Hydrolysis-Resistant Analogues of Cyclic ADP-ribose:  Modification of the “Northern” Ribose and Calcium Release Activity

Abstract: Three novel analogues modified in the "northern" ribose (ribose linked to N1 of adenine) of the Ca(2+) mobilizing second messenger cyclic adenosine diphosphoribose, termed 2"-NH(2)-cyclic adenosine diphosphoribose, cyclic adenosine diphospho-carbocyclic-ribose, and 8-NH(2)-cyclic adenosine diphospho-carbocyclic-ribose, were synthesized (chemoenzymatically and by total synthesis) and spectroscopically characterized, and the pK(a) values for the 6-amino/imino transition were determined in two cases. The biologic… Show more

“…However, to our surprise, it was inactive in T cells, whereas natural cADPR effectively mobilizes Ca 2+ in both neuronal cells and T cells. 34) These results confirmed that the target proteins and/or the mechanism of action of cADPR in sea urchin eggs, T cells, and neuronal cells are different, 35) as suggested by previous biological studies. [36][37][38][39][40][41][42] …”

Cyclic ADP-Carbocyclic-Ribose and -4-Thioribose, as Stable Mimics of Cyclic ADP-Ribose, a Ca²⁺-Mobilizing Second Messenger

“…However, to our surprise, it was inactive in T cells, whereas natural cADPR effectively mobilizes Ca 2+ in both neuronal cells and T cells. 34) These results confirmed that the target proteins and/or the mechanism of action of cADPR in sea urchin eggs, T cells, and neuronal cells are different, 35) as suggested by previous biological studies. [36][37][38][39][40][41][42] …”

Cyclic ADP-Carbocyclic-Ribose and -4-Thioribose, as Stable Mimics of Cyclic ADP-Ribose, a Ca²⁺-Mobilizing Second Messenger

“…In contrast, in mammalian cells, cADPcR acted much more weakly as compared to the sea urchin system (Guse et al, 2002). However, it was found that cIDPcR showed only an insignificant Ca 2þ -mobilizing effect (EC 50 > 10 6 mM), and 8-BrcIDPcR was almost inactive in sea urchin egg homogenates (Shuto and Matsuda, 2004).…”

Cyclic ADP‐Ribose Analogues with Minimal Structure: Synthesis and Calcium‐Release Activity

“…Permeabilized Jurkat T cells were prepared as detailed previously (14). In brief, cells were transferred into an intracellular medium (nominally Ca 2ϩ -free, pH 7.2), permeabilized with 55 mg/ml saponin for 20 min, and afterward washed three times to remove all saponin.…”

“…O-Methylation of the 3Ј-hydroxyl group generated an antagonist (12). The stable carbocyclic derivative cyclic aristeromycin diphosphoribose was an agonist in both sea urchin eggs and T lymphocytes (13,14). To further explore the structure-activity relationship of cADPR in mammalian cells, we replaced both the southern and northern ribose moieties of cIDPR with ether strands.…”

A Minimal Structural Analogue of Cyclic ADP-ribose