Self-assembly
provides researchers powerful tools for creating
ordered functional structures and complex architectures. Investigation
of in vivo self-assembly reveals the assembly/aggregation-induced
retention (AIR) effect and enhanced targeting effect, which can be
applied to promising biomedical applications by enhancing molecular
accumulation in the target region. These unique bioeffects inspire
the interest of researchers in construction of self-assembled nanomaterials
in biological systems. Although many efforts have been achieved, the
in-depth analysis of the relationship between assemblies and functions
is rarely reported. Here, we focus on the relationship of chlorophyll-derivative
assemblies and their photoacoustic signals and attempt to establish
a method for monitoring the aggregation efficiency in vivo based on
photoacoustic signals. Three arginine-rich peptide-purpurin molecules
were designed and synthesized. The assembled capabilities and assembly
processes of these molecules were characterized and monitored by UV,
fluorescence, and CD spectra images of gradually changing polarities
in mixed solvents, and the morphologies of the assemblies were observed
by TEM. Furthermore, the relationship between the aggregation ratios
of the molecules and the ratiometric photoacoustic signals was systemically
studied. We prospect that the fundamental research in revealing objective
laws will be useful for future guidance in optimizing photoacoustic
detection windows and assembled molecule design.
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