Essential and mutually compensatory roles of alpha-mannosidase II and alpha-mannosidase IIx in N-glycan processing in vivo in mice

Akama TO; Nakagawa H; Wong NK; Sutton-Smith M; Dell A; Morris HR; Nakayama J; Nishimura SI; Pai A; Moremen KW

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Essential and mutually compensatory roles of alpha-mannosidase II and alpha-mannosidase IIx in N-glycan processing in vivo in mice

机译：α-甘露糖苷酶II和α-甘露糖苷酶IIx在小鼠体内N-聚糖加工中的基本和相互补偿的作用

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Many proteins synthesized through the secretory pathway receive posttranslational modifications, including N-glycosylation. a-Mannosidase II (MII) is a key enzyme converting precursor high-mannose-type N-glycans to matured complex-type structures. Previous studies showed that Mll-null mice synthesize complextype N-glycans, indicating the presence of an alternative pathway. Because alpha-mannosiclase IN (MX) is a candidate enzyme for this pathway, we asked whether MX functions in N-glycan processing by generating MII/MX double-null mice. Some double-nulls died between embryonic days 15.5 and 18.5, but most survived until shortly after birth and died of respiratory failure, which represents a more severe phenotype than that seen in single-nulls for either gene. Structural analysis of N-glycans revealed that double-nulls completely lack complex-type N-glycans, demonstrating a critical role for at least one of these enzymes for effective N-glycan processing. Recombinant mouse MX and MII showed identical substrate specificities toward N-glycan substrates, suggesting that MX is an isozyme of MII. Thus, either MII or MX can biochemically compensate for the deficiency of the other in vivo, and either of two is required for late embryonic and early postnatal development.

机译：通过分泌途径合成的许多蛋白质都接受翻译后修饰，包括N-糖基化。 α-甘露糖苷酶II（MII）是将前体高甘露糖型N-聚糖转化为成熟的复杂类型结构的关键酶。先前的研究表明，Mll-null小鼠可合成复杂类型的N-聚糖，表明存在替代途径。因为α-甘露糖苷酶IN（MX）是该途径的候选酶，所以我们询问MX是否通过产生MII / MX双无效小鼠而在N-聚糖加工中起作用。一些双零位在胚胎的第15.5至18.5天之间死亡，但大多数存活到出生后不久并死于呼吸衰竭，这代表了比任一基因的单零位更严重的表型。 N-聚糖的结构分析表明，双无效分子完全缺乏复杂类型的N-聚糖，这表明这些酶中的至少一种对于N-聚糖的有效加工至关重要。重组小鼠MX和MII对N-聚糖底物表现出相同的底物特异性，这表明MX是MII的同工酶。因此，MII或MX都可以通过生物化学方法来弥补另一种体内缺陷，而后期胚胎发育和出生后早期发育则需要两者之一。

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来源
《Proceedings of the National Academy of Sciences of the United States of America》 |2006年第24期|p. 8983-8988|共6页
作者
Akama TO; Nakagawa H; Wong NK; Sutton-Smith M; Dell A; Morris HR; Nakayama J; Nishimura SI; Pai A; Moremen KW;
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作者单位

Burnham Inst Med Res, Canc Res Ctr, Glycobiol Program, La Jolla, CA 92037 USA;

Hokkaido Univ, Grad Sch Adv Life Sci, Frontier Res Ctr Post Genome Sci & Technol, Sapporo, Hokkaido 0010021, Japan;

Univ London Imperial Coll Sci & Technol, Biochem Div Mol Biosci, London SW7 2AZ, England;

Shinshu Univ, Sch Med, Dept Pathol, Matsumoto, Nagano 3908621, Japan;

Univ Georgia, Complex Carbohydrate Res Ctr, Athens, GA 30602 USA;

Univ Georgia, Dept Biochem & Mol Biol, Athens, GA 30602 USA;

Univ Calif San Diego, Howard Hughes Med Inst, Dept Cellular & Mol Med, La Jolla, CA 92093 USA;

M SCAN Mass Spectrometry Res & Training Ctr, Ascot SL5 7PZ, Berks, England;

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收录信息美国《科学引文索引》(SCI);美国《生物学医学文摘》(MEDLINE);美国《化学文摘》(CA);
原文格式 PDF
正文语种 eng
中图分类自然科学总论;
关键词
gene knockout; mutation; ASPARAGINE-LINKED OLIGOSACCHARIDES; BROAD-SPECIFICITY ALPHA-1-2; GLYCOSYLATION TYPE IIA; RAT-LIVER; SURFACTANT HOMEOSTASIS; CONGENITAL DISORDER; DEFICIENT MICE; BIOSYNTHESIS; PATHWAY; DISEASE;

机译：基因敲除;突变;天冬酰胺连接寡糖;通透性ALPHA-1- 2;糖基化类型IIA;大鼠-肝脏;表面稳态;先天性疾病;缺陷小鼠;生物合成;途径;疾病;
入库时间 2022-08-18 00:44:56

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机译：寻找选择性和有效的高尔基α-甘露糖苷酶II抑制剂作为潜在的抗癌药：3-取代-swainsonine类似物的合成和在固体支持物上固定的swainsonine类似物的制备。
6. Essential and mutually compensatory roles of α-mannosidase II and α-mannosidase IIx in N-glycan processing in vivo in mice [O] . Tomoya O. Akama, Hiroaki Nakagawa, Nyet Kui Wong, 2006

机译：α-甘露糖苷酶II和α-甘露糖苷酶IIx在小鼠体内N-聚糖加工中的基本和相互补偿作用
7. Essential and mutually compensatory roles of α-mannosidase II and α-mannosidase IIx in N-glycan processing in vivo in mice [O] . Akama, Tomoya O., Nakagawa, Hiroaki, Wong, Nyet Kui, 2006

机译：α-甘露糖苷酶II和α-甘露糖苷酶IIx在小鼠体内N-聚糖加工中的基本和相互补偿作用

Essential and mutually compensatory roles of alpha-mannosidase II and alpha-mannosidase IIx in N-glycan processing in vivo in mice

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