EXP001861

Paper

Cell penetrating peptide conjugated bioreducible polymer for siRNA delivery (2011)

Peptide

Sequence: C-YGRKKRRQRRR

RNA

All experiment fields

Experiment Id	EXP001861
Paper	Cell penetrating peptide conjugated bioreducible polymer for siRNA delivery
Peptide	Tat (HIV-1 Tat CPP) conjugated polymer
Delivery Success Class	no
In Vivo Flag	no
Uptake Confirmed	yes
Label Confidence	medium
In Vitro Functional Effect	yes
Endosomal Escape Evidence
Peptide Concentration	Polymer carrier; used as polyplex at weight ratio (polymer:siRNA) = 20 (key apoptosis/knockdown assays).
Rna Concentration	50 nM siRNA (key hypoxia apoptosis assays); SHP-1 screening also at 25–100 nM.
Mixing Ratio	Weight ratio (polymer:siRNA) = 20 (apoptosis assays); peptide-modified polymer mixed 1:1 with unmodified CD prior to complexation.
Formulation Format	Peptide-conjugated bioreducible polymer/siRNA polyplex
Formulation Components	Tat-CD (peptide-conjugated poly(CBA-DAH) (cystamine bisacrylamide–diaminohexane bioreducible polymer)) + siRNA \| Peptides (PCM and/or Tat) conjugated to poly(CBA-DAH) via SM(PEG)2; peptide-modified polymers mixed 1:1 with unmodified CD to form effective polyplexes.
Size Nm	115.40
Zeta Mv	23.20
Model Scope	in_vitro
Model Type	in vitro
Cell Lines Or Primary Cells	H9C2 rat cardiomyocytes (hypoxia-mimic CoCl2 + serum deprivation for apoptosis model)
Animal Model
Administration Route
Output Type	In vitro functional RNA effect: gene silencing + anti-apoptotic phenotype
Output Value	SHP-1 mRNA knockdown (qRT-PCR) and reduced apoptosis under hypoxia (Annexin V/PI; increased MTT viability; reduced LDH).
Output Units
Output Notes	SHP-1 siRNA no.2 gave strongest knockdown; PCM+Tat polyplex gave strongest suppression and anti-apoptotic effect.
Toxicity Notes	MTT/LDH indicate improved viability and reduced cytotoxicity under hypoxia with SHP-1 or Fas siRNA polyplexes vs controls.
Curation Notes