Kicska Greg A, Tyler Peter C, Evans Gary B, Furneaux Richard H, Shi Wuxian, Fedorov Alexander, Lewandowicz Andrzej, Cahill Sean M, Almo Steven C, Schramm Vern L
Department of Biochemistry, Albert Einstein College of Medicine, 1300 Morris Park Avenue, Bronx, New York 10461, USA.
Biochemistry. 2002 Dec 10;41(49):14489-98. doi: 10.1021/bi026636f.
Immucillin-H (ImmH) and immucillin-G (ImmG) were previously reported as transition-state analogues for bovine purine nucleoside phosphorylase (PNP) and are the most powerful inhibitors reported for the enzyme (K(i) = 23 and 30 pM). Sixteen new immucillins are used to probe the atomic interactions that cause tight binding for bovine PNP. Eight analogues of ImmH are identified with equilibrium dissociation constants of 1 nM or below. A novel crystal structure of bovine PNP-ImmG-PO(4) is described. Crystal structures of ImmH and ImmG bound to bovine PNP indicate that nearly every H-bond donor/acceptor site on the inhibitor is fully engaged in favorable H-bond partners. Chemical modification of the immucillins is used to quantitate the energetics for each contact at the catalytic site. Conversion of the 6-carbonyl oxygen to a 6-amino group (ImmH to ImmA) increases the dissociation constant from 23 pM to 2.6 million pM. Conversion of the 4'-imino group to a 4'-oxygen (ImmH to 9-deazainosine) increases the dissociation constant from 23 pM to 2.0 million pM. Substituents that induce small pK(a) changes at N-7 demonstrate modest loss of affinity. Thus, 8-F or 8-CH(3)-substitutions decrease affinity less than 10-fold. But a change in the deazapurine ring to convert N-7 from a H-bond donor to a H-bond acceptor (ImmH to 4-aza-3-deaza-ImmH) decreases affinity by >10(7). Introduction of a methylene bridge between 9-deazahypoxanthine and the iminoribitol (9-(1'-CH(2))-ImmH) increased the distance between leaving and oxacarbenium groups and increased K(i) to 91 000 pM. Catalytic site energetics for 20 substitutions in the transition-state analogue are analyzed in this approach. Disruption of the H-bond pattern that defines the transition-state ensemble leads to a large decrease in binding affinity. Changes in a single H-bond contact site cause up to 10.1 kcal/mol loss of binding energy, requiring a cooperative H-bond pattern in binding the transition-state analogues. Groups involved in leaving group activation and ribooxacarbenium ion stabilization are central to the H-bond network that provides transition-state stabilization and tight binding of the immucillins.
免疫菌素-H(ImmH)和免疫菌素-G(ImmG)此前被报道为牛嘌呤核苷磷酸化酶(PNP)的过渡态类似物,是该酶已知的最强抑制剂(K(i) = 23和30 pM)。16种新的免疫菌素用于探究导致与牛PNP紧密结合的原子间相互作用。鉴定出8种ImmH类似物,其平衡解离常数为1 nM或更低。描述了牛PNP-ImmG-PO(4)的一种新晶体结构。ImmH和ImmG与牛PNP结合的晶体结构表明,抑制剂上几乎每个氢键供体/受体位点都与有利的氢键伙伴充分结合。对免疫菌素进行化学修饰以定量催化位点处每次接触的能量。将6-羰基氧转化为6-氨基(ImmH转化为ImmA)使解离常数从23 pM增加到260万pM。将4'-亚氨基转化为4'-氧(ImmH转化为9-脱氮肌苷)使解离常数从23 pM增加到200万pM。在N-7处引起小的pK(a)变化的取代基显示出亲和力适度丧失。因此,8-F或8-CH(3)取代使亲和力降低不到10倍。但是将脱氮嘌呤环改变以使N-7从氢键供体变为氢键受体(ImmH转化为4-氮杂-3-脱氮-ImmH)使亲和力降低>10(7)。在9-脱氮次黄嘌呤和亚氨基核糖醇之间引入亚甲基桥(9-(1'-CH(2))-ImmH)增加了离去基团和氧杂碳鎓离子之间的距离,并使K(i)增加到91000 pM。用这种方法分析了过渡态类似物中20种取代的催化位点能量。破坏定义过渡态集合的氢键模式导致结合亲和力大幅降低。单个氢键接触位点的变化导致结合能损失高达10.1 kcal/mol,这需要在结合过渡态类似物时形成协同氢键模式。参与离去基团活化和核糖氧杂碳鎓离子稳定的基团对于提供过渡态稳定和免疫菌素紧密结合的氢键网络至关重要。
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