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Targeting Visceral Fat by Intraperitoneal Delivery of Novel AAV Serotype Vector Restricting Off-Target Transduction in Liver  Wei Huang, Xianglan Liu,

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Presentation on theme: "Targeting Visceral Fat by Intraperitoneal Delivery of Novel AAV Serotype Vector Restricting Off-Target Transduction in Liver  Wei Huang, Xianglan Liu,"— Presentation transcript:

1 Targeting Visceral Fat by Intraperitoneal Delivery of Novel AAV Serotype Vector Restricting Off-Target Transduction in Liver  Wei Huang, Xianglan Liu, Nicholas J. Queen, Lei Cao  Molecular Therapy - Methods & Clinical Development  Volume 6, Pages (September 2017) DOI: /j.omtm Copyright © 2017 The Author(s) Terms and Conditions

2 Molecular Therapy - Methods & Clinical Development 2017 6, 68-78DOI: (10.1016/j.omtm.2017.06.002)
Copyright © 2017 The Author(s) Terms and Conditions

3 Figure 1 i.p. Administration of Rec2 Vector Transduces Multiple Visceral Fat Depots (A) Representative in vivo bioluminescence imaging of luciferase 2 weeks after i.p. Rec2-luciferase vector injection (2 × 1010 vg per mouse). (B) GFP content in tissue lysates of mice receiving Rec2-GFP (1 × 1010 vg per mouse) 2 weeks after i.p. injection. (C) GFP immunohistochemistry in mice receiving Rec2-GFP (1 × 1010 vg per mouse). Scale bar, 100 μm. Molecular Therapy - Methods & Clinical Development 2017 6, 68-78DOI: ( /j.omtm ) Copyright © 2017 The Author(s) Terms and Conditions

4 Figure 2 i.p. Administration of Dual-Cassette AS/Rec2 Vector Selectively Transduces Visceral Fat while Restricting Off-Target Transgene Expression in Liver (A) Schematic of the AAV vectors. The liver-restricted vector contains two expression cassettes: one to express transgene under the non-selective CBA promoter, the other to express a microRNA targeting WPRE driven by the liver-specific albumin (Alb) promoter, thereby preventing transgene expression in the liver. (B) GFP content in tissue lysates of mice receiving i.p. injection of AS/Rec2-GFP at indicated doses of one experiment 2 weeks after i.p. injection. (C) GFP content in tissue lysates in another dose-response experiment 2 weeks after i.p. injection. Data are mean ± SEM, n = 3 to 4 per group. (D) Viral vector genomic copy numbers in selected tissues 2 weeks after i.p. administration of AS/Rec2-GFP (4 × 1010 vg per mouse). Molecular Therapy - Methods & Clinical Development 2017 6, 68-78DOI: ( /j.omtm ) Copyright © 2017 The Author(s) Terms and Conditions

5 Figure 3 i.p. Administration of AS/Rec2-Leptin Vector Rescues the Leptin-Deficient Phenotype of ob/ob Mice (A) Body weight. (B) Weigh gain. (C) Representative picture 9 weeks after AAV injection. (D) Cumulative food intake. (E) Rectal temperature. At a 4-week time point, body temperature was measured after a 6-hr fast. (F) EchoMRI analysis of body composition 4 weeks after AAV injection. Data are mean ± SEM, n = 6 per group. ***p < Molecular Therapy - Methods & Clinical Development 2017 6, 68-78DOI: ( /j.omtm ) Copyright © 2017 The Author(s) Terms and Conditions

6 Figure 4 AS/Rec2-Leptin Treatment Corrects Impaired Glucose Tolerance and Disturbance of Energy Balance in ob/ob Mice (A) Serum leptin level 4 weeks after AAV injection. Leptin undetectable in AS/Rec2-GFP-treated ob/ob mice. (B) Glucose tolerance test 4 weeks after AAV injection. ***p < for AS/Rec2-leptin-treated ob/ob mice and WT mice compared to AS/Rec2-GFP-treated ob/ob mice. At 0 min and 60 min, glucose levels in AS/Rec2-leptin-treated ob/ob mice were significantly lower than those in WT mice (p < 0.05). (C) Body weight at glucose tolerance test. (D) Cumulative food. (E) Oxygen consumption; p < (F) Physical activity was measured by Comprehensive Lab Animal Monitoring System (CLAMS) 5 weeks after AAV injection, p < Shaded area, dark phase. Data are mean ± SEM, n = 6 AS/Rec2-GFP, n = 6 AS/Rec2-leptin, and n = 6–8 age-matched WT mice. Molecular Therapy - Methods & Clinical Development 2017 6, 68-78DOI: ( /j.omtm ) Copyright © 2017 The Author(s) Terms and Conditions

7 Figure 5 AS/Rec2-Leptin Treatment Reverses Obesity, Hyperinsulinemia, and Liver Steatosis in ob/ob Mice (A) Relative tissue weight at sacrifice 9 weeks after AAV injection. (B) Serum insulin level at sacrifice. Data are means ± SEM. n = 6 per group. ∗∗∗ p < (C) Oil red O staining of livers. Scale bar, 50 μm. (D) GFP content in tissue lysates of an individual ob/ob mouse receiving AS/Rec2-GFP. Molecular Therapy - Methods & Clinical Development 2017 6, 68-78DOI: ( /j.omtm ) Copyright © 2017 The Author(s) Terms and Conditions

8 Figure 6 Leptin Levels in ob/ob Mice Treated with Unrestricted Single Cassette Leptin Vector or Liver-Restricted Dual Cassette AS/Rec2-Leptin Vector at Sacrifice 9 Weeks after AAV Injection (A) Leptin level in eWAT lysates. (B) Leptin level in liver lysates. (C) Leptin level in serum. Data are mean ± SEM, n = 5 unrestricted Rec2-leptin, n = 6 liver-restricted AS/Rec2-leptin, and n = 4 age-matched WT mice. *p < 0.05; ***p < Molecular Therapy - Methods & Clinical Development 2017 6, 68-78DOI: ( /j.omtm ) Copyright © 2017 The Author(s) Terms and Conditions

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