Current Faculty

	R. Rox Anderson
	Brett E. Bouma
	Apostolos G. Doukas
	Michael R. Hamblin
	Tayyaba Hasan
	Irene E. Kochevar
	Seemantini Nadkarni
	Charles P. Lin
	Robert W. Redmond
	Guillermo J. Tearney
	Hensin Tsao
	Benjamin Vakoc
	Robert H. Webb
	Mei X. Wu
	Anna Yaroslavsky
	Seok-Hyun (Andy) Yun

Visiting Faculty

Former Faculty

Research Staff

Administration

Macrophage-targeted PDT

Conjugates between PS and modified albumin can be readily and specifically taken up by macrophages via the high capacity scavenger receptor. Tumor associated macrophages (TAMs) can be selectively killed or modified by the appropriate PDT regimen. It has become apparent in recent years that TAMs are partly responsible for the growth, invasion and metastasis of tumors and are therefore a valid target for cancer therapy. This may be accomplished by a binary approach in which the PS-conjugate targets the macrophages and the spatial confinement of the light delivery ensures that only TAMs (bad) are killed and other macrophages (good) are spared. We are studying the correlation between precise conjugate structure and scavenger receptor subtypes (SRA or CD36). The long-term goal is to be able to specifically target certain macrophage phenotypes and activation state for photodestruction.

Hamblin MR, Miller, JL, Ortel B. Scavenger-receptor targeted photodynamic therapy. Photochem Photobiol 2000;72(4):533-40.

Demidova TN, Hamblin MR. Macrophage targeted photodynamic therapy. Int J Immunopathol Pharmacol 2004; 17(2):117-26.

Liu Q, Hamblin MR. Macrophage-targeted photodynamic therapy: scavenger receptor expression and activation state. Int J Immunopathol Pharmacol. 2005, 18: 391-402.