¹H NMR spectroscopy was utilized to study the host–guest recognition between CB[7] and DOX. Because DOX is insoluble in aqueous solution, 3-methylcyclohexylamine was used as a model guest. As shown in Figure 1D, when equimolar amounts of CB[7] and 3-methylcyclohexylamine were mixed in D₂O, obvious chemical shift changes of the protons on 3-methylcyclohexylamine were observed, suggesting that 3-methylcyclohexylamine was encapsulated in the hydrophobic cavity of CB[7]. When three equivalents of 3-methylcyclohexylamine were added into CB[7], the peak shape of 3-methylcyclohexylamine became similar to that of free 3-methylcyclohexylamine (Figure 1C), suggesting that there were excess free 3-methylcyclohexylamine in solution. On the other hand, nuclear Overhauser effect correlation signals between CB[7] and 3-methylcyclohexylamine were observed (Supplementary Figure S2), further demonstrating host–guest complexation occurred between CB[7] and 3-methylcyclohexylamine, in which the guest molecular deeply penetrated into the cavity of CB[7].

Isothermal titration calorimetry (ITC) was used to acquire the thermodynamic information for the complexation between CB[7] and 3-methylcyclohexylamine. As shown in Supplementary Figure S3, the K _a values of CB[7]⊃3-methylcyclohexylamine were determined to be (2.73 ± 0.84) × 10⁶ M⁻¹, indicating the binding affinity was very high and was favorable for the fabrication of supramolecular systems in physiological environments. Furthermore, the enthalpy changes (ΔH < 0) indicated that the host–guest recognition between CB[7] and 3-methylcyclohexylamine was driven by enthalpy changes. All these results indicated that the complexation between CB[7] and DOX could take place via host–guest interactions, which paved the way for the construction of supramolecular nanomedicine.

After confirming the possible inclusion complexation between CB[7] and DOX, we studied the morphology of supramolecular nanomedicines in water. As can be seen in Figure 2A, large precipitates were observed in the DOX group owing to the low solubility of DOX in water, but regular spherical nanoparticles with a diameter of about 100 nm were observed in the presence of CB[7] (Figure 2B), suggesting hydrophilic CB[7] significantly inhibited the π–π stacking and improved the water solubility of DOX. The average diameter of CB[7]⊃DOX measured by the dynamic light scattering (DLS) experiment was 121 ± 13.4 nm (Figure 2C), which is in accordance with the result from transmission electron microscopy (TEM). The average diameter of the supramolecular nanomedicine almost remained unchanged after incubation in PBS for 48 h (Figures 2D, 4E), implying that the stability of supramolecular nanomedicine was good in the physiological environment.

The internalization behavior of CB[7]⊃DOX was then studied by confocal laser scanning microscopy (CLSM). As shown in Figure 3A, obvious red fluorescence arising from DOX was observed in the cytoplasm after 2 h incubation, proving that CB[7]⊃DOX was easily internalized by HeLa cells. When incubation time reached 4 h, the red fluorescence appeared in both the cytoplasm and nucleus, suggesting that CB[7]⊃DOX could enter into the nucleus to prime their therapeutic actions. The endocytic pathways of supramolecular nanomedicines were evaluated by adding different endocytosis inhibitors, such as amiloride-HCl (AMD), chlorpromazine (CPZ), and genistein (Gen). As shown in Figures 3B, 4F, the internalization of supramolecular nanomedicines was greatly inhibited at 4°C, indicating their cell uptake was energy-dependent. Meanwhile, pre-treatment with CPZ, AMD, or Gen led to the difference in decrease of cellular uptakes, suggesting that the endocytosis of nanomedicines was mediated by the cooperation of clathrin-, micropinocytosis-, and caveolae-participated endocytic pathways.

The therapeutic efficacy of supramolecular nanomedicines against U87 and HeLa cells was assessed by a 3-(4′,5′-dimethylthiazol-2′-yl)-2,5-diphenyltetrazolium bromide (MTT) assay. The IC₅₀ values of CB[7]⊃DOX against U87 and HeLa cells were 12.5 ± 1.43 and 11.9 ± 1.24 μM, respectively, which were comparable to the IC₅₀ values of DOX (6.52 ± 0.70 and 5.47 ± 0.68 μM against U87 and HeLa cells, respectively) (Figure 3C and Supplementary Figure S4). An Annexin V-FITC/propidium iodide (PI) dual-staining assay was utilized to analyze the percentage of apoptotic cells. Figure 4H showed that a large percentage of the apoptotic (31.3%) and necrotic (7.8%) cells was monitored for the HeLa cells treated with CB[7]⊃DOX, which was similar to the values for the cells treated with free DOX. CB[7]⊃DOX also showed a similar ability to induce the apoptosis of U87 cells (Supplementary Figure S6), further demonstrating the anticancer efficacy of DOX was fully kept after supramolecular fabrication. The percentage of apoptotic cells induced by CB[7]⊃DOX was also higher than that in the free DOX group (Figure 3D and Supplementary Figure S6), suggesting the anticancer activity of DOX was highly maintained.

Apart from DOX, CB[7] could also be used as a host to interact with CPT through molecular recognition. The host−guest interaction between CB[7] and CPT was verified by biolayer interferometry (Supplementary Figure S7), which demonstrated that CPT could be stably encapsulated by CB[7] due to the high binding affinity. More interestingly, the host−guest complexation was able to regulate the self-assembly of CPT. Due to the severe π–π stacking interactions, CPT formed large aggregates in aqueous solution (Figure 4A). By the formation of the host−guest inclusion complex, CB[7]⊃CPT self-assembled into nanoparticles (Figure 4B). The average diameter of the obtained nanoparticles was measured to be 133 ± 17.2 nm by DLS (Figure 4C). The solubility of CPT is extremely poor, which was determined to be 10.3 ± 0.87 μg/ml in PBS. It should be emphasized that the solubility of CPT greatly increased in the presence of CB[7] (Figure 4D) because water soluble CB[7] encapsulated CPT and significantly inhibited the π–π stacking of CPT. Additionally, the stability of the nanoparticles formed by CB[7]⊃CPT was satisfactory, and negligible changes in the size of the assemblies were detected by DLS over 48 h (Figure 4E). Similar to CB[7]⊃DOX, the endocytosis of nanoparticles assembled from CB[7]⊃CPT was also mediated by the cooperation of clathrin-, micropinocytosis-, and caveolae-participated endocytic pathways. The anticancer capability of CB[7]⊃CPT was evaluated by an MTT assay, which indicated that the IC₅₀ value of CB[7]⊃CPT was lower than that of free CPT. The possible reason was that the aggregates formed from free CPT were unfavorable for cellular internalization, while the supramolecular modification optimized the size of assemblies prepared from CB[7]⊃CPT, thus enhancing cell uptake. Annexin V-FITC/PI dual staining further demonstrated that the therapeutic efficacy of CPT was fully maintained after supramolecular fabrication (Figures 4H,I).