Zahid Maliha, Weber Beth, Yurko Ray, Islam Kazi, Agrawal Vaishavi, Lopuszynski Jack, Yagi Hisato, Salama Guy
Dept. of Cardiovascular Diseases, Mayo Clinic, Rochester, MN.
Pittsburgh Heart, Lung, Blood, and Vascular Medicine Institute and Division of Cardiology, Department of Medicine, University of Pittsburgh School of Medicine and University of Pittsburgh Medical Center, Pittsburgh, PA, USA.
bioRxiv. 2023 May 10:2023.05.10.540206. doi: 10.1101/2023.05.10.540206.
Amiodarone is underutilized due to significant off-target toxicities. We hypothesized that targeted delivery to the heart would lead to lowering of dose by utilizing a cardiomyocyte targeting peptide (CTP), a cell penetrating peptide identified by our prior phage display work.
CTP was synthesized thiolated at the N-terminus, conjugated to amiodarone via Schiff base chemistry, HPLC purified and confirmed with MALDI/TOF. Stability of the conjugate was assessed using serial HPLCs. Guinea pigs (GP) were injected intraperitoneally daily with vehicle (7 days), amiodarone (7 days; 80mg/Kg), CTP-amiodarone (5 days;26.3mg/Kg), or CTP (5 days; 17.8mg/Kg), after which GPs were euthanized, hearts excised, perfused on a Langendorff apparatus with Tyrode's solution and blebbistatin (5μM) to minimize contractions. Voltage (RH237) and Ca -indicator dye (Rhod-2/AM) were injected, fluorescence from the epicardium split and focused on two cameras capturing at 570-595nm for cytosolic Ca and 610-750nm wavelengths for voltage. Subsequently, hearts were paced at 250ms with programmed stimulation to measure changes in conduction velocities (CV), action potential duration (APD) and Ca transient durations at 90% recovery (CaTD ). mRNA was extracted from all hearts and RNA sequencing performed with results compared to control hearts.
CTP-amiodarone remained stable for up to 21 days at 37°C. At ∼1/15 of the dose of amiodarone, CTP-amiodarone decreased CV in hearts significantly compared to control GPs (0.92±0.05 vs. 1.00±0.03m/s, p=0.0007), equivalent to amiodarone alone (0.87±0.08ms, p=0.0003). Amiodarone increased APD (192±5ms vs. 175±8ms for vehicle, p=0.0025), while CTP-amiodarone decreased it significantly (157±16ms, p=0.0136) similar to CTP alone (155±13ms, p=0.0039). Both amiodarone and CTP-amiodarone significantly decreased calcium transients compared to controls. CTP-amiodarone and CTP decreased CaTD to an extent greater than amiodarone alone (p<0.001). RNA-seq showed that CTP alone increased the expression of DHPR and SERCA2a, while decreasing expression of proinflammatory genes NF-kappa B, TNF-α, IL-1β, and IL-6.
Our data suggests that CTP can deliver amiodarone to cardiomyocytes at ∼1/15 the total molar dose of amiodarone needed to produce comparable slowing of CVs. The ability of CTP to decrease AP durations and CaTD may be related to its increase in expression of Ca-handling genes, and merits further study.
由于显著的非靶向毒性,胺碘酮的使用未得到充分利用。我们推测,通过利用心肌细胞靶向肽(CTP)进行靶向心脏递送,可利用我们之前通过噬菌体展示工作鉴定出的一种细胞穿透肽来降低剂量。
CTP在N端合成硫醇化,通过席夫碱化学与胺碘酮偶联,经高效液相色谱(HPLC)纯化并用基质辅助激光解吸电离/飞行时间质谱(MALDI/TOF)确认。使用系列HPLC评估偶联物的稳定性。豚鼠(GP)每天腹腔注射赋形剂(7天)、胺碘酮(7天;80mg/Kg)、CTP-胺碘酮(5天;26.3mg/Kg)或CTP(5天;17.8mg/Kg),之后对豚鼠实施安乐死,切除心脏,在Langendorff装置上用台氏液和blebbistatin(5μM)灌注以尽量减少收缩。注入电压(RH237)和钙指示剂染料(Rhod-2/AM),将心外膜的荧光分离并聚焦于两台相机,一台在57
