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Fragment crystallizable region
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The fragment crystallizable region ( Fc region) is the tail region of an that interacts with cell surface receptors called and some proteins of the complement system. This region allows antibodies to activate the , for example, through binding to . In , and antibody isotypes, the Fc region is composed of two identical protein fragments, derived from the second and third constant domains of the antibody's two heavy chains; and Fc regions contain three heavy chain constant domains (CH domains 2–4) in each chain.

(2025). 9780815336426, Garland Publishing. .
(1988). 9780849360787, Crc Press. .
The Fc regions of IgGs bear a highly conserved N-glycosylation site. of the Fc fragment is essential for Fc receptor-mediated activity. The attached to this site are predominantly core- diantennary structures of the complex type. In addition, small amounts of these N-glycans also bear bisecting GlcNAc and α-2,6 linked residues.

The other part of an antibody, called the , contains variable sections that define the specific target that the antibody can bind. By contrast, the Fc region of all antibodies in a class are the same for each species; they are constant rather than variable. The Fc region is, therefore, sometimes incorrectly termed the "fragment constant region".

Fc binds to various cell receptors and complement proteins. In this way, it mediates different effects of antibodies (detection of opsonized particles; cell ; of , , and ; and other processes).

(2025). 9781451117837, Lippincott Williams & Wilkins. .


Engineered Fc fragments
In a new development in the field of antibody-based therapeutics, the Fc region of has been engineered to contain an -binding site. This type of antigen-binding fragment is called . Fcab fragments can be inserted into a full immunoglobulin by swapping the Fc region, thus obtaining a bispecific antibody (with both Fab and Fcab regions containing distinct binding sites). These bispecific monoclonal antibodies are sometimes referred to as mAb2.


See also

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