TY - JOUR
T1 - Adenovirus-mediated gene therapy for corneal clouding in mice with mucopolysaccharidosis type VII
AU - Kamata, Yuko
AU - Okuyama, Torayuki
AU - Kosuga, Motomichi
AU - O'hira, Aya
AU - Kanaji, Arihiko
AU - Sasaki, Kyoko
AU - Yamada, Masao
AU - Azuma, Noriyuki
N1 - Funding Information:
We thank Yumi Kanegae and Izumu Saito (Institute of Medical Science, University of Tokyo) for recombinant adenovirus constructs. This work was supported in part by grants for pediatric research from Ministry of Health, Labor, and Welfare Japan.
PY - 2001
Y1 - 2001
N2 - Recent advances in systemic treatments for mucopolysaccharidosis have led to therapies that improve the multiple somatic features of this disease, but the therapeutic effect on ocular manifestations such as corneal clouding is not satisfactory. Here, we administered an adenovirus expressing human β-glucuronidase (AxCAhGUS) into the anterior chamber or intrastromal region of the cornea in mice with mucopolysaccharidosis type VII (B6/MPSVII), and successfully treated corneal clouding of MPSVII. When we injected AxCAhGUS into the anterior chamber of the eyes, cells expressing β-glucuronidase (GUSB) were located mainly in the trabecular meshwork as well as in all corneal regions, and subsequent pathological corrections in the cornea were achieved. Widespread transgene expression was also observed when we administered AxCAhGUS inside the cornea after lamellar keratotomy, and rapid elimination of the lysosomal storage in the corneal keratocytes occurred. Furthermore, intrastromal vector administration did not generate significant levels of anti-adenovirus neutralizing antibodies, and secondary vector administration was effective. Based on these observations, we conclude that it is worth developing a treatment strategy for corneal clouding in mucopolysaccharidosis based on direct intraocular administration of adenoviral vectors.
AB - Recent advances in systemic treatments for mucopolysaccharidosis have led to therapies that improve the multiple somatic features of this disease, but the therapeutic effect on ocular manifestations such as corneal clouding is not satisfactory. Here, we administered an adenovirus expressing human β-glucuronidase (AxCAhGUS) into the anterior chamber or intrastromal region of the cornea in mice with mucopolysaccharidosis type VII (B6/MPSVII), and successfully treated corneal clouding of MPSVII. When we injected AxCAhGUS into the anterior chamber of the eyes, cells expressing β-glucuronidase (GUSB) were located mainly in the trabecular meshwork as well as in all corneal regions, and subsequent pathological corrections in the cornea were achieved. Widespread transgene expression was also observed when we administered AxCAhGUS inside the cornea after lamellar keratotomy, and rapid elimination of the lysosomal storage in the corneal keratocytes occurred. Furthermore, intrastromal vector administration did not generate significant levels of anti-adenovirus neutralizing antibodies, and secondary vector administration was effective. Based on these observations, we conclude that it is worth developing a treatment strategy for corneal clouding in mucopolysaccharidosis based on direct intraocular administration of adenoviral vectors.
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U2 - 10.1006/mthe.2001.0461
DO - 10.1006/mthe.2001.0461
M3 - Article
C2 - 11592832
AN - SCOPUS:0034756448
SN - 1525-0016
VL - 4
SP - 307
EP - 312
JO - Molecular Therapy
JF - Molecular Therapy
IS - 4
ER -