About: Human natural antibodies to mammalian carbohydrate antigens (MCA) bind to carbohydrate-antigens synthesized in other mammalian species and protect against zoonotic virus infections. Three such anti-MCA antibodies are: (1) anti-Gal, also produced in Old-World monkeys and apes, binds to α-gal epitopes synthesized in non-primate mammals, lemurs, and New-World monkeys; (2) anti-Neu5Gc binds to Neu5Gc (N-glycolyl-neuraminic acid) synthesized in apes, Old-World monkeys, and many non-primate mammals; and (3) anti-Forssman binds to Forssman-antigen synthesized in various mammals. Anti-viral protection by anti-MCA antibodies is feasible because carbohydrate chains of virus envelopes are synthesized by host glycosylation machinery and thus are similar to those of their mammalian hosts. Analysis of MCA glycosyltransferase genes suggests that anti-Gal appeared in ancestral Old-World primates following catastrophic selection processes in which parental populations synthesizing α-gal epitopes were eliminated in enveloped virus epidemics. However, few mutated offspring in which the α1,3galactosyltransferase gene was accidentally inactivated produced natural anti-Gal that destroyed viruses presenting α-gal epitopes, thereby preventing extinction of mutated offspring. Similarly, few mutated hominin offspring that ceased to synthesize Neu5Gc produced anti-Neu5Gc, which destroyed viruses presenting Neu5Gc synthesized in parental hominin populations. A present-day example for few humans having mutations that prevent synthesis of a common carbohydrate antigen (produced in >99.99% of humans) is blood-group Bombay individuals with mutations inactivating H-transferase; thus, they cannot synthesize blood-group O (H-antigen) but produce anti-H antibody. Anti-MCA antibodies prevented past extinctions mediated by enveloped virus epidemics, presently protect against zoonotic-viruses, and may protect in future epidemics. Travelers to regions with endemic zoonotic viruses may benefit from vaccinations elevating protective anti-MCA antibody titers.

Facets (new session)
Description
Metadata
Settings
- owl:sameAs
- Inference Rule:

About: Human natural antibodies to mammalian carbohydrate antigens (MCA) bind to carbohydrate-antigens synthesized in other mammalian species and protect against zoonotic virus infections. Three such anti-MCA antibodies are: (1) anti-Gal, also produced in Old-World monkeys and apes, binds to α-gal epitopes synthesized in non-primate mammals, lemurs, and New-World monkeys; (2) anti-Neu5Gc binds to Neu5Gc (N-glycolyl-neuraminic acid) synthesized in apes, Old-World monkeys, and many non-primate mammals; and (3) anti-Forssman binds to Forssman-antigen synthesized in various mammals. Anti-viral protection by anti-MCA antibodies is feasible because carbohydrate chains of virus envelopes are synthesized by host glycosylation machinery and thus are similar to those of their mammalian hosts. Analysis of MCA glycosyltransferase genes suggests that anti-Gal appeared in ancestral Old-World primates following catastrophic selection processes in which parental populations synthesizing α-gal epitopes were eliminated in enveloped virus epidemics. However, few mutated offspring in which the α1,3galactosyltransferase gene was accidentally inactivated produced natural anti-Gal that destroyed viruses presenting α-gal epitopes, thereby preventing extinction of mutated offspring. Similarly, few mutated hominin offspring that ceased to synthesize Neu5Gc produced anti-Neu5Gc, which destroyed viruses presenting Neu5Gc synthesized in parental hominin populations. A present-day example for few humans having mutations that prevent synthesis of a common carbohydrate antigen (produced in >99.99% of humans) is blood-group Bombay individuals with mutations inactivating H-transferase; thus, they cannot synthesize blood-group O (H-antigen) but produce anti-H antibody. Anti-MCA antibodies prevented past extinctions mediated by enveloped virus epidemics, presently protect against zoonotic-viruses, and may protect in future epidemics. Travelers to regions with endemic zoonotic viruses may benefit from vaccinations elevating protective anti-MCA antibody titers. Goto Sponge NotDistinct Permalink

An Entity of Type : fabio:Abstract, within Data Space : wasabi.inria.fr associated with source document(s)

Attributes	Values
type	abstract
value	Human natural antibodies to mammalian carbohydrate antigens (MCA) bind to carbohydrate-antigens synthesized in other mammalian species and protect against zoonotic virus infections. Three such anti-MCA antibodies are: (1) anti-Gal, also produced in Old-World monkeys and apes, binds to α-gal epitopes synthesized in non-primate mammals, lemurs, and New-World monkeys; (2) anti-Neu5Gc binds to Neu5Gc (N-glycolyl-neuraminic acid) synthesized in apes, Old-World monkeys, and many non-primate mammals; and (3) anti-Forssman binds to Forssman-antigen synthesized in various mammals. Anti-viral protection by anti-MCA antibodies is feasible because carbohydrate chains of virus envelopes are synthesized by host glycosylation machinery and thus are similar to those of their mammalian hosts. Analysis of MCA glycosyltransferase genes suggests that anti-Gal appeared in ancestral Old-World primates following catastrophic selection processes in which parental populations synthesizing α-gal epitopes were eliminated in enveloped virus epidemics. However, few mutated offspring in which the α1,3galactosyltransferase gene was accidentally inactivated produced natural anti-Gal that destroyed viruses presenting α-gal epitopes, thereby preventing extinction of mutated offspring. Similarly, few mutated hominin offspring that ceased to synthesize Neu5Gc produced anti-Neu5Gc, which destroyed viruses presenting Neu5Gc synthesized in parental hominin populations. A present-day example for few humans having mutations that prevent synthesis of a common carbohydrate antigen (produced in >99.99% of humans) is blood-group Bombay individuals with mutations inactivating H-transferase; thus, they cannot synthesize blood-group O (H-antigen) but produce anti-H antibody. Anti-MCA antibodies prevented past extinctions mediated by enveloped virus epidemics, presently protect against zoonotic-viruses, and may protect in future epidemics. Travelers to regions with endemic zoonotic viruses may benefit from vaccinations elevating protective anti-MCA antibody titers.
subject	Immunology Zoonoses Immune system Biomolecules Nutrition Antibodies Carbohydrates Animal diseases Mammals Glycoproteins Bathonian first appearances Extant Middle Jurassic first appearances Reagents for biochemistry Taxa named by Carl Linnaeus
part of	Human Natural Antibodies to Mammalian Carbohydrate Antigens as Unsung Heroes Protecting against Past, Present, and Future Viral Infections
is abstract of	Human Natural Antibodies to Mammalian Carbohydrate Antigens as Unsung Heroes Protecting against Past, Present, and Future Viral Infections
is hasSource of	covid:ann/target/c8ef3126b0eb3c75f5df721f7b781f45003d363a covid:ann/target/9faf2818006263167414baaba94b1e35c1c0a4b8 covid:ann/target/6ff078bc9afd8f5763db4c97710a5370001df29c covid:ann/target/3a15077c8a2d0e2a4335850d31963f4e99431dc4 covid:ann/target/0b84fa3b6d305f602fefefd3c5fc2ea72221e97d covid:ann/target/e2fad52473c22c4b812bfbad532f56b1d099d143 covid:ann/target/b63e0055345b14becd0d82f62f49b058f9413cdb covid:ann/target/02bf5b90f9fded1964b3c136d6da9b881f4005d9 covid:ann/target/49793634961650e27f3a7c6e43c2d3c2e49f7ccc covid:ann/target/f26bf435424a5117b48bf5508d907bb5d7e39b84 covid:ann/target/29af1b285fc765443a27709a9be7cc5f1c65ca91 covid:ann/target/4e041d85ae2b8c9d799ac2b79b5103ee7a552b25 covid:ann/target/557a210da815e93645ab6e19a8d8253008e95311 covid:ann/target/dbaeb2992379ae2074b4cf25779d9d0b00718b7d covid:ann/target/a502c1b49826284918f4eb0742d7fb4ab75500d8 covid:ann/target/07f78fe56161d5ee735eaa63bcb4be4c3ba4a251 covid:ann/target/a897e52cd6557a605906d9764a5975d7da72f91f covid:ann/target/3a50b10232f83be22cbb3fb303a8a24c329f5857 covid:ann/target/967783407362f47f44b73c38cfeeac577611aeb0 covid:ann/target/95c4c48e44a3763e9f9e09cbc02c7efe7d8d3318 covid:ann/target/926abfb517c0b480b5b7183375fc24cc4bedb931 covid:ann/target/b5e9f626f5ecf3be4180b4e28d3575fc5499106f covid:ann/target/f4fcde553003579dbedf18ff43ad46b1b11ab943 covid:ann/target/c0d8ec27f9796c3ccfbed77ff2d65a9fef076b7b covid:ann/target/7596fc419e814c179ee27df77415090271f2115a covid:ann/target/c6b32b69ba7751a9250c5c5c74f7df3072a56d67 covid:ann/target/1c80a14769294ffcff01aaccd236ed7a24bc47bd covid:ann/target/8602c8f69a5d37822921d2e3b20189a54cb799ee covid:ann/target/b00e8bf98630d76b7188c78374ba61cc77c2ae21

Faceted Search & Find service v1.13.91 as of Mar 24 2020

Alternative Linked Data Documents: Sponger | ODE Content Formats:

RDF

ODATA

Microdata

About

OpenLink Virtuoso version 07.20.3229 as of Jul 10 2020, on Linux (x86_64-pc-linux-gnu), Single-Server Edition (94 GB total memory)
Data on this page belongs to its respective rights holders.
Virtuoso Faceted Browser Copyright © 2009-2025 OpenLink Software