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早期卵巢切除术揭示了由发育性O-连接N-乙酰半乳糖胺糖基化产生的天然抗A和抗Tn交叉反应性免疫球蛋白M(IgM)的种系编码。(种系编码的天然抗A/抗Tn交叉反应性IgM)

Early ovariectomy reveals the germline encoding of natural anti-A- and Tn-cross-reactive immunoglobulin M (IgM) arising from developmental O-GalNAc glycosylations. (Germline-encoded natural anti-A/Tn cross-reactive IgM).

作者信息

Arend Peter

机构信息

Philipps University Marburg, Department of Medicine, D-355 Marburg/Lahn, Germany.

Gastroenterology Research Laboratory, University of Iowa, College of Medicine, Iowa City, Iowa.

出版信息

Cancer Med. 2017 Jul;6(7):1601-1613. doi: 10.1002/cam4.1079. Epub 2017 Jun 5.

Abstract

While native blood group A-like glycans have not been demonstrated in prokaryotic microorganisms as a source of human "natural" anti-A isoagglutinin production, and metazoan eukaryotic N-acetylgalactosamine O-glycosylation of serine or threonine residues (O-GalNAc-Ser/Thr-R) does not occur in bacteria, the O-GalNAc glycan-bearing ovarian glycolipids, discovered in C57BL/10 mice, are complementary to the syngeneic anti-A-reactive immunoglobulin M (IgM), which is not present in animals that have undergone ovariectomy prior to the onset of puberty. These mammalian ovarian glycolipids are complementary also to the anti-A/Tn cross-reactive Helix pomatia agglutinin (HPA), a molluscan defense protein, emerging from the coat proteins of fertilized eggs and reflecting the snail-intrinsic, reversible O-GalNAc glycosylations. The hexameric structure of this primitive invertebrate defense protein gives rise to speculation regarding an evolutionary relationship to the mammalian nonimmune, anti-A-reactive immunoglobulin M (IgM) molecule. Hypothetically, this molecule obtains its complementarity from the first step of protein glycosylations, initiated by GalNAc via reversible O-linkages to peptides displaying Ser/Thr motifs, whereas the subsequent transferase depletion completes germ cell maturation and cell renewal, associated with loss of glycosidic bonds and release of O-glycan-depleted proteins, such as complementary IgM revealing the structure of the volatilely expressed "lost" glycan carrier through germline Ser residues. Consequently, the evolutionary/developmental first glycosylations of proteins appear metabolically related or identical to that of the mucin-type, potentially "aberrant" monosaccharide GalNAcα1-O-Ser/Thr-R, also referred to as the Tn (T "nouvelle") antigen, and explain the anti-Tn cross-reactivity of human innate or "natural" anti-A-specific isoagglutinin and the pronounced occurrence of cross-reactive anti-Tn antibody in plasma from humans with histo-blood group O. In fact, A-allelic, phenotype-specific GalNAc glycosylation of plasma proteins does not occur in human blood group O, affecting anti-Tn antibody levels, which may function as a growth regulator that contributes to a potential survival advantage of this group in the overall risk of developing cancer when compared with non-O blood groups.

摘要

虽然原核微生物中尚未证实存在与人类“天然”抗A同种凝集素产生相关的天然血型A样聚糖,且细菌中不存在后生动物真核生物中丝氨酸或苏氨酸残基的N - 乙酰半乳糖胺O - 糖基化(O - GalNAc - Ser/Thr - R),但在C57BL/10小鼠中发现的带有O - GalNAc聚糖的卵巢糖脂,与同基因的抗A反应性免疫球蛋白M(IgM)互补,而在青春期前接受卵巢切除术的动物中不存在这种IgM。这些哺乳动物卵巢糖脂也与抗A/Tn交叉反应的滨螺凝集素(HPA)互补,HPA是一种软体动物防御蛋白,源自受精卵的外壳蛋白,反映了蜗牛内在的、可逆的O - GalNAc糖基化。这种原始无脊椎动物防御蛋白的六聚体结构引发了关于其与哺乳动物非免疫性、抗A反应性免疫球蛋白M(IgM)分子进化关系的推测。假设该分子的互补性源于蛋白质糖基化的第一步,由GalNAc通过可逆的O - 连接与显示Ser/Thr基序的肽段结合起始,而随后的转移酶缺失完成生殖细胞成熟和细胞更新,这与糖苷键的丧失和O - 聚糖缺失蛋白的释放相关,例如互补性IgM通过种系Ser残基揭示挥发性表达的“丢失”聚糖载体的结构。因此,蛋白质的进化/发育首次糖基化在代谢上似乎与粘蛋白型、潜在“异常”的单糖GalNAcα1 - O - Ser/Thr - R(也称为Tn(“新”T)抗原)相关或相同,并解释了人类先天或“天然”抗A特异性同种凝集素的抗Tn交叉反应性以及O血型人群血浆中明显出现的交叉反应性抗Tn抗体。事实上,人类O血型中血浆蛋白不存在A等位基因、表型特异性的GalNAc糖基化,这影响了抗Tn抗体水平,抗Tn抗体可能作为一种生长调节因子,与非O血型相比,在O血型人群患癌总体风险中可能有助于其潜在的生存优势。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8060/5504323/443de875aead/CAM4-6-1601-g001.jpg

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