| Identification | Back Directory | [Name]
CPHPC | [CAS]
224624-80-0 | [Synonyms]
CPHPC
Miridesap
Ro63-8695
GSK2315698
CPOHPC acid
CPHPC(Miridesap)
CPOHPC (acid form
CPHPC, Ro-63-8695
GSK2315698,Miridesap
CPHPC(GSK2315698,Miridesap)
1,1'-(1,6-Dioxo-1,6-hexanediyl)bis[D-proline]
D-Proline, 1,1'-(1,6-dioxo-1,6-hexanediyl)bis-
MIRIDESAP; RO-638695; RO 638695; RO638695;CPHPC;CPOHPC (ACID FORM; CPOHPC ACID | [Molecular Formula]
C16H24N2O6 | [MDL Number]
MFCD09970762 | [MOL File]
224624-80-0.mol | [Molecular Weight]
340.37 |
| Chemical Properties | Back Directory | [storage temp. ]
Sealed in dry,2-8°C | [solubility ]
≤30mg/ml in ethanol;20mg/ml in DMSO;25mg/ml in dimethyl formamide | [form ]
crystalline solid | [color ]
White to off-white |
| Hazard Information | Back Directory | [Description]
Serum amyloid P (SAP) is pentraxin with roles in inflammation and immune response. CPHPC is a divalent crosslinker of SAP that causes rapid depletion of circulating SAP via hepatic clearance. It also produces significant reduction of SAP from cerebrospinal fluid and visceral amyloid deposits. CPHPC has been used with anti-SAP antibodies to eliminate amyloid deposits in clinical trials of systemic amyloidosis. | [Uses]
Miridesap is a potential drug in the treatment of amyloidosis. | [in vitro]
previous study found that the multi-point binding of cphpc between pairs of pentameric sap molecules increased the avidity of the interaction, and this was reflected in an apparent affinity constant of 10 nm. moreover, the x-ray crystal structure of the sap–cphpc complex confirmed that it was a decamer composed of two pentameric sap molecules reversibly crosslinked by five cphpc molecules [1]. | [in vivo]
mice were received cphpc at 1 mg/ml in their drinking water for the rest of the experiment. circulating human sap was depleted but significant amounts of sap remained in the amyloid deposits. five days after starting on cphpc, one group received a single intraperitoneal injection of 50 mg of the igg fraction of sheep anti-human sap antiserum, containing 7 mg of anti-sap antibody. a control group received 50 mg of unrelated sheep igg. the third group received no treatment and thus controlled for spontaneous regression of aa amyloid. results showed that there was dramatically less amyloid after treatment with cphpc plus anti-sap antibody than in the other two groups but there was no difference between cphpc alone and no treatment [2]. | [References]
[1] m. b. pepys, j. herbert, w. l. hutchinson, et al. targeted pharmacological depletion of serum amyloid p component for treatment of human amyloidosis. nature 417, 254-259 (2002).
[2] k. bodin, s. ellmerich, m. c. kahan, et al. antibodies to human serum amyloid p component eliminate visceral amyloid deposits. nature 468, 93-97 (2010).
[3] gillmore jd et al. ustained pharmacological depletion of serum amyloid p component in patients with systemic amyloidosis. br j haematol. 2010 mar;148(5):760-7. |
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| Company Name: |
DC Chemicals
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| Tel: |
021-58447131 13564518121 |
| Website: |
http://www.approvedhomemanagement.com/ShowSupplierProductsList927327/0.htm |
| Company Name: |
Wuhan Topule
|
| Tel: |
+86-02787215551 +86-19945035818 |
| Website: |
http://www.topule.com/ |
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