Compositions and methods related to engineered Fc constructs

The invention claimed is: 1. An Fc construct comprising: a) a first polypeptide having the formula A-L-B; wherein i) A comprises a first Fc domain monomer; ii) L is a linker; and iii) B comprises a second Fc domain monomer; b) a second polypeptide having the formula A′-L′-B′; wherein i) A′ comprises a third Fc domain monomer; ii) L′ is a linker; and iii. B′ comprises a fourth Fc domain monomer; c) a third polypeptide comprises a fifth Fc domain monomer; and d) a fourth polypeptide comprises a sixth Fc domain monomer; wherein the A of first polypeptide and the A′ of second polypeptide combine to form a first Fc domain, the B of first polypeptide and fifth Fc domain monomer combine to form a second Fc domain, and the B′ of second polypeptide and sixth Fc domain monomer combine to form a third Fc domain; and wherein the first Fc domain monomer and the third Fc domain monomer comprise complementary dimerization selectivity modules that promote dimerization between the first Fc domain monomer and the third Fc domain monomer; second Fc domain monomer and the fifth Fc domain monomer comprise complementary dimerization selectivity modules that promote dimerization between the second Fc domain monomer and the fifth Fc domain monomer; the fourth Fc domain monomer and the sixth Fc domain monomer comprise complementary dimerization selectivity modules that promote dimerization between the fourth Fc domain monomer and the sixth Fc domain monomer; wherein each of A, B, A′, B′, the third polypeptide and the fourth polypeptide comprises an Fc domain monomer; and each Fc domain monomer comprises a hinge domain, a C H 2 domain and a C H 3 domain; and wherein at least one of the Fc domain monomers comprises both a S267E mutation and a L328F mutation that together enhance binding to the FcγRIIb receptor. 2. A method of treating inflammation in a subject, the method comprising administering to the subject a pharmaceutical composition comprising therapeutically effective amount of an Fc construct of claim 1 . 3. The Fc construct of claim 1 , further comprising an albumin-binding peptide comprising SEQ ID NO: 28. 4. The Fc construct of claim 1 , wherein the first polypeptide and the second polypeptide have the same amino acid sequence and wherein the third polypeptide and the fourth polypeptide have the same amino acid sequence. 5. The Fc construct of claim 1 , wherein each Fc domain monomers comprises both a S267E mutation and a L328F mutation. 6. The Fc construct of claim 1 , wherein each of the first, second, third and fourth polypeptides lack a carboxy-terminal lysine. 7. The Fc construct of claim 1 , wherein each dimerization selectivity module independently comprises: (a) an engineered cavity in the C H 3 domain of one of the Fc domain monomers and an engineered protuberance in the C H 3 domain of the other of the Fc domain monomers, wherein the engineered cavity and the engineered protuberance are positioned to form a protuberance-into-cavity pair of Fc domain monomers; or (b) a negatively-charged amino acid in the C H 3 domain of one of the domain monomers and a positively-charged amino acid in the C H 3 domain of the other of the Fc domain monomers, wherein the negatively-charged amino acid and the positively-charged amino acid are positioned to promote formation of an Fc domain.