Schematic representation of essential MRAP regions. Shown are MRAP regions that appear to be required for dual topology and for two functions: facilitating MC2 receptor trafficking to the plasma membrane, and facilitating MC2 receptor binding.

Specificity of MRAP bimolecular fluorescence complementation. A, live CHO cells transfected with MRAP fused to YFP fragments on opposite sides or the same side of the MRAP protein. B, live CHO cells transfected with V5-MRAP-YFP-F2 and Gβ₁-YFP-F1, YFP-F1-V5-MRAP, and Gγ₇-YFP-F2, or Gβ₁-YFP-F1 and Gγ₇-YFP-F2 as shown. Left panels, YFP fluorescence. Right panels, surface expression of MRAP detected by staining live cells with anti-V5 antibody.

The anti-parallel homodimeric structure of MRAP is achieved in the ER. A, schematic representation of configurations in which the YFP fragments fused to MRAP or RAMP molecules interact in the cell. B, surface MC2 receptor was detected by ELISA using anti-HA antibody in nonpermeabilized CHO cells expressing MC2 receptor with an NH₂-terminal HA tag and RAMP1, YFP-F1-V5-MRAP, V5-MRAP-YFP-F2, or both. C, live CHO cells transfected with MRAP or RAMP1 fused to YFP fragments as shown. Left panels, YFP fluorescence. Right panels, surface expression of MRAP detected using anti-V5 antibody. D, live CHO cells transfected with YFP-F1-V5-MRAP and V5-MRAP-YFP-F2 and stained with ER-tracker. ^*, p < 0.05 versus RAMP1 control.

Regions of MRAP required for MC2 receptor trafficking and signaling. HA-MC2 receptor was expressed in CHO cells with empty vector (MC2R alone), RAMP3, MRAP, or MRAP mutants. A, C, E, and G, surface HA-MC2 receptor was detected in nonpermeabilized cells by ELISA using anti-HA antibody. B, D, F, and H, cAMP concentration following incubation with 0.1 mm isobutylmethylxanthine and 100 nm ACTH for 20 min. Results for MRAPct are from Ref. 6. Data are expressed as percent of the value obtained with full-length MRAP. ^*, p < 0.05 versus RAMP3 control.

Effect of MRAP on ¹²⁵I-ACTH binding to MC2 receptor. CHO cells were transfected with no receptor (Mock) or HA-MC2 receptor and RAMP3, MRAP, or MRAP(18-21A). A, surface expression of HA-MC2 receptor measured by ELISA using anti-HA antibody. B, ¹²⁵I-ACTH binding. The bar on the far right depicts cells incubated with 1 μm unlabeled ACTH for 20 min before and during the 1-h binding assay. C, competition displacement measured in cells incubated with ¹²⁵I-ACTH (300,000 cpm/ml, ∼0.1 nm) and unlabeled ACTH at the concentrations shown. ^*, p < 0.01 versus RAMP3 control.

Structure and function of mMRAP2. A, sequence of mMRAP2 cloned from mouse adrenal gland cDNA. B, surface staining of live CHO cells expressing V5-mMRAP2-Flag with anti-V5 (top) or anti-FLAG (bottom) antibodies is shown in green; nuclei are counterstained in blue. C, CHO cells were transfected with HA-MC2 receptor and RAMP3, MRAP, mMRAP2, or mMRAP2 with LDYI inserted after residue 28 as shown. Surface HA-MC2 receptor was detected by ELISA in nonpermeabilized cells using anti-HA antibody. D, cAMP concentration in CHO cells expressing HA-MC2 receptor and RAMP3 or MRAP constructs shown following incubation with 0.1 mm isobutylmethylxanthine and 100 nm ACTH for 20 min. Data in C and D are expressed as percent of the value obtained with full-length MRAP. ^*, p < 0.05 versus RAMP3 (C) or vehicle (D).

Amino acids 31 to 37 of MRAP are required for dual topology. A, amino acid sequence of mouse MRAP. The predicted transmembrane domain is underlined, and the single natural potential N-linked glycosylation site is shown in bold. B, left panel, schematic representation of constructs studied. Right panels, surface expression of NH₂-(V5) and/or COOH-terminal (FLAG) epitopes measured by ELISA in nonpermeabilized CHO cells using anti-V5 or anti-FLAG antibodies. Results for MRAPct are from Ref. 6. C, surface staining of live CHO cells expressing V5-RAMP3-Flag, V5-MRAP-Flag, or V5-MRAPΔ31-37-Flag with anti-V5 (top) or anti-FLAG (bottom) antibodies (shown in green); nuclei are counterstained in blue. D, live CHO cells expressing YFP-F1-V5-MRAP and V5-MRAP-YFP-F2 or the equivalent constructs of MRAPΔ31-37. Left panels show YFP fluorescence and right panels show surface MRAP visualized by staining live cells with anti-V5 antibody. E, CHO cells transfected with V5-MRAP-Flag or V5-MRAPΔ31-37-Flag were incubated with anti-V5 plus anti-FLAG antibodies. Immunoprecipitates (IP) were resolved on SDS-PAGE and the blot probed with anti-FLAG antibody. Filled and open circles show mobility of glycosylated and nonglycosylated species determined after PNGase digestion (6). F, cells expressing MRAP-V5 and MRAP-Flag or equivalent constructs of MRAPΔ31-37 were lysed and anti-V5 or anti-FLAG antibody was added. Immunoprecipitates were resolved on SDS-PAGE and blots probed with anti-V5 or anti-FLAG antibody. G, cells were transfected with V5-RAMP3-Flag or V5-RAMP3(MRAP29-37)-Flag. NH₂- or COOH-terminal epitopes on the surface of nonpermeabilized cells were detected by ELISA using anti-V5 or anti-FLAG antibodies. Overall expression of V5-RAMP3(MRAP29-37)-Flag was comparable with that of V5-RAMP3-Flag, but surface expression was lower. In panels B and F, data are normalized to surface expression of the NH₂-terminal V5 epitope for each construct. ^*, p < 0.01 versus RAMP3 control.