Increasing the electron density in BF2-coodinated azo compounds through para-substitution leads to a bathochromic shift in their activation wavelength. When the substituent is dimethyl amine, or the like, the trans/cis isomerization process can be efficiently modulated using near infrared light. The electron donating capability of the substituent also controls the hydrolysis half-life of the switch in aqueous solution, which is drastically longer for the cis isomer, while the BF2-coodination prevents reduction by glutathione.