Antigen binding molecule formats

What is claimed is: 1. A bispecific antigen-binding molecule comprising: (a) a first polypeptide chain comprising in an N-to-C terminal orientation: (i) a first Fc domain; and (ii) a first Fab domain that binds to a cytokine and comprises a first heavy chain variable region (VH) domain associated with a first light chain variable region (VL) domain; and (b) a second polypeptide chain comprising in an N-to-C terminal orientation: (i) a second Fc domain associated with the first Fc domain to form an Fc heterodimer; and (ii) a second Fab domain that is non-identical to the first Fab domain, binds to the cytokine, and comprises a second VH domain associated with a second VL domain; (c) a third polypeptide chain associated with the first polypeptide, the third polypeptide comprising in an N-to-C terminal orientation: (i) the first VL domain; and (ii) a first constant domain of the light chain (CL) domain; and (d) a fourth polypeptide chain associated with the second polypeptide, the fourth polypeptide comprising in an N-to-C terminal orientation: (i) the second VL domain; and (ii) a second CL domain, wherein the first Fab domain and the second Fab domain are the only antigen-binding domains in the antigen-binding molecule. 2. The antigen-binding molecule of claim 1 , which comprises a first linker between the first Fc domain and the first VH domain and a second linker between the second Fc domain and the second VH domain. 3. The antigen-binding molecule of claim 2 , wherein the first linker and the second linker have identical amino acid sequences. 4. The antigen-binding molecule of claim 1 , wherein the first polypeptide chain comprises a first hinge domain N-terminal to the first Fc domain and the second polypeptide chain comprises a second hinge domain N-terminal to the second Fc domain. 5. The antigen-binding molecule of claim 1 , which has one hinge region. 6. The antigen-binding molecule of claim 1 , which has two hinge regions. 7. The antigen-binding molecule of claim 1 , wherein the Fc domains in the Fc heterodimer comprise knob-in-hole mutations as compared to a wild type Fc domain. 8. A pharmaceutical composition comprising the antigen-binding molecule of claim 1 and an excipient. 9. The antigen-binding molecule of claim 1 , which is complexed at a 1:1 ratio with the cytokine. 10. The antigen-binding molecule of claim 1 , wherein the cytokine is thymic stromal lymphopoietin (TSLP), IL-1α, IL-1β, IL-12, IL-18, TNFα, IL-23, IL-13, macrophage migration inhibitory factor (MIF), IL-6, IL-17, IL-20, IL-15, IL-9, IL-4, IL-5, IL-25, TGF-β, CCL25. 11. The antigen-binding molecule of claim 1 , wherein the cytokine is human thymic stromal lymphopoietin (TSLP).