Peptide Information
General Information of This Peptide
| Peptide ID |
PEP00039
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|---|---|---|---|---|---|---|
| Peptide Name |
PDIP
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| Structure |
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| Sequence |
GCGGPLYKKIIKKLLESGG-Azidoalanine-GGAPLYKKIIKKLCES
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| Peptide Type |
Cyclic
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| Receptor Name |
Phosphatidylserine lipid headgroups
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Receptor Info | ||||
| PDC Transmembrane Types | Cell-penetrating peptides (CPPs) | |||||
| Formula |
C172H291N47O45S2
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| Isosmiles |
[H]NCCCC[C@@H]1NC(=O)[C@H](Cc2ccc(O[H])cc2)NC(=O)[C@H](CC(C)C)NC(=O)[C@@H]2CCCN2C(=O)CNC(=O)CNC(=O)[C@@H](NC(=O)CN[H])CSSC[C@@H](C(=O)N[C@@H](CCC(=O)O)C(=O)N[C@@H](CO[H])C(=O)O)NC(=O)[C@H](CC(C)C)NC(=O)[C@H](CCCCN[H])NC(=O)[C@H](CCCCN[H])NC(=O)[C@]([H])([C@@H](C)CC)NC(=O)[C@]([H])([C@@H](C)CC)NC(=O)[C@H](CCCCN[H])NC(=O)[C@H](CCCCN[H])NC(=O)[C@H](Cc2ccc(O[H])cc2)NC(=O)[C@H](CC(C)C)NC(=O)[C@@H]2CCCN2C(=O)[C@H](C)NC(=O)CNC(=O)CNC(=O)[C@H](CN=[N+]=[N-])NC(=O)CNC(=O)CNC(=O)[C@H](CO[H])NC(=O)[C@H](CCC(=O)O)NC(=O)[C@H](CC(C)C)NC(=O)[C@H](CC(C)C)NC(=O)[C@H](CCCCN[H])NC(=O)[C@H](CCCCN[H])NC(=O)[C@]([H])([C@@H](C)CC)NC(=O)[C@]([H])([C@@H](C)CC)NC(=O)[C@H](CCCCN[H])NC1=O
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| InChI |
InChI=1S/C172H291N47O45S2/c1-20-98(15)140-167(258)201-111(46-28-36-68-177)149(240)193-109(44-26-34-66-175)151(242)203-118(75-94(7)8)158(249)205-117(74-93(5)6)157(248)199-115(60-62-138(231)232)153(244)210-125(89-220)145(236)187-84-133(226)184-87-136(229)191-124(82-189-217-182)144(235)186-83-132(225)183-86-135(228)190-102(19)171(262)219-73-41-51-130(219)166(257)209-121(78-97(13)14)160(251)207-123(80-104-54-58-106(223)59-55-104)163(254)198-108(43-25-33-65-174)148(239)196-114(49-31-39-71-180)156(247)214-143(101(18)23-4)170(261)216-141(99(16)21-2)168(259)202-112(47-29-37-69-178)150(241)194-110(45-27-35-67-176)152(243)204-119(76-95(9)10)161(252)212-128(164(255)200-116(61-63-139(233)234)154(245)211-126(90-221)172(263)264)92-266-265-91-127(192-131(224)81-181)146(237)188-85-134(227)185-88-137(230)218-72-40-50-129(218)165(256)208-120(77-96(11)12)159(250)206-122(79-103-52-56-105(222)57-53-103)162(253)197-107(42-24-32-64-173)147(238)195-113(48-30-38-70-179)155(246)213-142(100(17)22-3)169(260)215-140/h52-59,93-102,107-130,140-143,220-223H,20-51,60-92,173-181H2,1-19H3,(H,183,225)(H,184,226)(H,185,227)(H,186,235)(H,187,236)(H,188,237)(H,190,228)(H,191,229)(H,192,224)(H,193,240)(H,194,241)(H,195,238)(H,196,239)(H,197,253)(H,198,254)(H,199,248)(H,200,255)(H,201,258)(H,202,259)(H,203,242)(H,204,243)(H,205,249)(H,206,250)(H,207,251)(H,208,256)(H,209,257)(H,210,244)(H,211,245)(H,212,252)(H,213,246)(H,214,247)(H,215,260)(H,216,261)(H,231,232)(H,233,234)(H,263,264)/t98-,99-,100-,101-,102-,107-,108-,109-,110-,111-,112-,113-,114-,115-,116-,117-,118-,119-,120-,121-,122-,123-,124-,125-,126-,127-,128-,129-,130-,140-,141-,142-,143-/m0/s1
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| InChIKey |
QZWGXIGNYFPFJM-XDYYLVNKSA-N
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| Pharmaceutical Properties |
Molecule Weight
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3801.638
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Polar area
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1476.68
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Complexity
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3799.136862
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xlogp Value
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-9.4186
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Heavy Count
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266
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Rot Bonds
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84
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Hbond acc
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54
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Hbond Donor
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49
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Each Peptide-drug Conjugate Related to This Peptide
Full Information of The Activity Data of The PDC(s) Related to This Peptide
PDIP-DBCO-SS-PQ [Investigative]
Obtained from the Model Organism Data
| Experiment 1 Reporting the Activity Data of This PDC | [1] | ||||
| Indication | Malaria | ||||
| Efficacy Data | Half Maximal Inhibitory Concentration (IC50) |
4.25 µM
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| Administration Time | 18-24 h | ||||
| Evaluation Method | Flow cytometry assay | ||||
| MOA of PDC |
As a proof of concept, we aimed to produce first-generation PDCs by conjugating the antimalarial drug primaquine (PQ) onto PDIP. Although PQ is one of the few drugs without clinically relevant resistance, it does not have widespread use because it causes hemolysis in individuals who are deficient in glucose-6-phosphate dehydrogenase (G6PD), a genetic trait common in malaria-endemic areas. Furthermore, PQ is metabolized into carboxyprimaquine in the body, which does not have any activity against the parasite. The proposed PDC approach provides the potential to deliver PQ directly to the parasite, which could prevent its interaction with healthy tissues and slow the conversion of PQ into inactive byproducts. Further, the combination of the peptide and drug, each with distinct antiplasmodial mechanisms of action, provides the potential to avoid the formation of drug-resistant parasites. Herein, we report the design, synthesis, and biological evaluation of a library of PDIP-PQ conjugates. Various design elements of the PDCs were probed to investigate their effect on biological activity, including: (i) the location of the PDIP conjugation site, (ii) the hydrophilicity of the linker between the peptide and drug, (iii) the spacing between the peptide and drug, and (iv) whether the linker can be cleaved to release the drug cargo under conditions which mimic the intracellular environment of infected RBCs. This work demonstrates that conjugation within the flexible interhelix spacer of PDIP and incorporation of traceless cleavable linkersbearing either a disulfide or trioxolane moietyare important for maintaining the low micromolar potency of the PQ drug cargo against P. falciparum.
Click to Show/Hide
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| Description |
The six PDIP-PQ conjugates were analyzed for their ability to inhibit the in vitro growth of P. falciparum asexual blood stage parasites (strain 3D7) in RBCs and were compared to the activity of the parent drug and peptide. We were encouraged to discover that most of the PDIP-PQ PDCs retained antiplasmodial activity similar to PDIP, with IC50 values in the low micromolar range. Notably, the various design elements probed provided valuable information regarding which PDC characteristics can be modified to improve activity.
Click to Show/Hide
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| In Vivo Model | Plasmodium falciparum 3D7. | ||||
| Half life period | 4.55 h | ||||
PDIP-DBCO-triox-PQ [Investigative]
Obtained from the Model Organism Data
| Experiment 1 Reporting the Activity Data of This PDC | [1] | ||||
| Indication | Malaria | ||||
| Efficacy Data | Half Maximal Inhibitory Concentration (IC50) |
4.68 µM
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| Administration Time | 18-24 h | ||||
| Evaluation Method | Flow cytometry assay | ||||
| MOA of PDC |
As a proof of concept, we aimed to produce first-generation PDCs by conjugating the antimalarial drug primaquine (PQ) onto PDIP. Although PQ is one of the few drugs without clinically relevant resistance, it does not have widespread use because it causes hemolysis in individuals who are deficient in glucose-6-phosphate dehydrogenase (G6PD), a genetic trait common in malaria-endemic areas. Furthermore, PQ is metabolized into carboxyprimaquine in the body, which does not have any activity against the parasite. The proposed PDC approach provides the potential to deliver PQ directly to the parasite, which could prevent its interaction with healthy tissues and slow the conversion of PQ into inactive byproducts. Further, the combination of the peptide and drug, each with distinct antiplasmodial mechanisms of action, provides the potential to avoid the formation of drug-resistant parasites. Herein, we report the design, synthesis, and biological evaluation of a library of PDIP-PQ conjugates. Various design elements of the PDCs were probed to investigate their effect on biological activity, including: (i) the location of the PDIP conjugation site, (ii) the hydrophilicity of the linker between the peptide and drug, (iii) the spacing between the peptide and drug, and (iv) whether the linker can be cleaved to release the drug cargo under conditions which mimic the intracellular environment of infected RBCs. This work demonstrates that conjugation within the flexible interhelix spacer of PDIP and incorporation of traceless cleavable linkersbearing either a disulfide or trioxolane moietyare important for maintaining the low micromolar potency of the PQ drug cargo against P. falciparum.
Click to Show/Hide
|
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| Description |
The six PDIP-PQ conjugates were analyzed for their ability to inhibit the in vitro growth of P. falciparum asexual blood stage parasites (strain 3D7) in RBCs and were compared to the activity of the parent drug and peptide. We were encouraged to discover that most of the PDIP-PQ PDCs retained antiplasmodial activity similar to PDIP, with IC50 values in the low micromolar range. Notably, the various design elements probed provided valuable information regarding which PDC characteristics can be modified to improve activity.
Click to Show/Hide
|
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| In Vivo Model | Plasmodium falciparum 3D7. | ||||
| Half life period | 3.99 h | ||||
PDIP-PEG3-PQ [Investigative]
Obtained from the Model Organism Data
| Experiment 1 Reporting the Activity Data of This PDC | [1] | ||||
| Indication | Malaria | ||||
| Efficacy Data | Half Maximal Inhibitory Concentration (IC50) |
8.81 µM
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| Administration Time | 18-24 h | ||||
| Evaluation Method | Flow cytometry assay | ||||
| MOA of PDC |
As a proof of concept, we aimed to produce first-generation PDCs by conjugating the antimalarial drug primaquine (PQ) onto PDIP. Although PQ is one of the few drugs without clinically relevant resistance, it does not have widespread use because it causes hemolysis in individuals who are deficient in glucose-6-phosphate dehydrogenase (G6PD), a genetic trait common in malaria-endemic areas. Furthermore, PQ is metabolized into carboxyprimaquine in the body, which does not have any activity against the parasite. The proposed PDC approach provides the potential to deliver PQ directly to the parasite, which could prevent its interaction with healthy tissues and slow the conversion of PQ into inactive byproducts. Further, the combination of the peptide and drug, each with distinct antiplasmodial mechanisms of action, provides the potential to avoid the formation of drug-resistant parasites. Herein, we report the design, synthesis, and biological evaluation of a library of PDIP-PQ conjugates. Various design elements of the PDCs were probed to investigate their effect on biological activity, including: (i) the location of the PDIP conjugation site, (ii) the hydrophilicity of the linker between the peptide and drug, (iii) the spacing between the peptide and drug, and (iv) whether the linker can be cleaved to release the drug cargo under conditions which mimic the intracellular environment of infected RBCs. This work demonstrates that conjugation within the flexible interhelix spacer of PDIP and incorporation of traceless cleavable linkersbearing either a disulfide or trioxolane moietyare important for maintaining the low micromolar potency of the PQ drug cargo against P. falciparum.
Click to Show/Hide
|
||||
| Description |
The six PDIP-PQ conjugates were analyzed for their ability to inhibit the in vitro growth of P. falciparum asexual blood stage parasites (strain 3D7) in RBCs and were compared to the activity of the parent drug and peptide. We were encouraged to discover that most of the PDIP-PQ PDCs retained antiplasmodial activity similar to PDIP, with IC50 values in the low micromolar range. Notably, the various design elements probed provided valuable information regarding which PDC characteristics can be modified to improve activity.
Click to Show/Hide
|
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| In Vivo Model | Plasmodium falciparum 3D7. | ||||
PDIP-PEG1-PQ [Investigative]
Obtained from the Model Organism Data
| Experiment 1 Reporting the Activity Data of This PDC | [1] | ||||
| Indication | Malaria | ||||
| Efficacy Data | Half Maximal Inhibitory Concentration (IC50) |
11.3 µM
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| Administration Time | 18-24 h | ||||
| Evaluation Method | Flow cytometry assay | ||||
| MOA of PDC |
As a proof of concept, we aimed to produce first-generation PDCs by conjugating the antimalarial drug primaquine (PQ) onto PDIP. Although PQ is one of the few drugs without clinically relevant resistance, it does not have widespread use because it causes hemolysis in individuals who are deficient in glucose-6-phosphate dehydrogenase (G6PD), a genetic trait common in malaria-endemic areas. Furthermore, PQ is metabolized into carboxyprimaquine in the body, which does not have any activity against the parasite. The proposed PDC approach provides the potential to deliver PQ directly to the parasite, which could prevent its interaction with healthy tissues and slow the conversion of PQ into inactive byproducts. Further, the combination of the peptide and drug, each with distinct antiplasmodial mechanisms of action, provides the potential to avoid the formation of drug-resistant parasites. Herein, we report the design, synthesis, and biological evaluation of a library of PDIP-PQ conjugates. Various design elements of the PDCs were probed to investigate their effect on biological activity, including: (i) the location of the PDIP conjugation site, (ii) the hydrophilicity of the linker between the peptide and drug, (iii) the spacing between the peptide and drug, and (iv) whether the linker can be cleaved to release the drug cargo under conditions which mimic the intracellular environment of infected RBCs. This work demonstrates that conjugation within the flexible interhelix spacer of PDIP and incorporation of traceless cleavable linkersbearing either a disulfide or trioxolane moietyare important for maintaining the low micromolar potency of the PQ drug cargo against P. falciparum.
Click to Show/Hide
|
||||
| Description |
The six PDIP-PQ conjugates were analyzed for their ability to inhibit the in vitro growth of P. falciparum asexual blood stage parasites (strain 3D7) in RBCs and were compared to the activity of the parent drug and peptide. We were encouraged to discover that most of the PDIP-PQ PDCs retained antiplasmodial activity similar to PDIP, with IC50 values in the low micromolar range. Notably, the various design elements probed provided valuable information regarding which PDC characteristics can be modified to improve activity.
Click to Show/Hide
|
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| In Vivo Model | Plasmodium falciparum 3D7. | ||||
PDIP-alk-PQ [Investigative]
Obtained from the Model Organism Data
| Experiment 1 Reporting the Activity Data of This PDC | [1] | ||||
| Indication | Malaria | ||||
| Efficacy Data | Half Maximal Inhibitory Concentration (IC50) |
12.9 µM
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| Administration Time | 18-24 h | ||||
| Evaluation Method | Flow cytometry assay | ||||
| MOA of PDC |
As a proof of concept, we aimed to produce first-generation PDCs by conjugating the antimalarial drug primaquine (PQ) onto PDIP. Although PQ is one of the few drugs without clinically relevant resistance, it does not have widespread use because it causes hemolysis in individuals who are deficient in glucose-6-phosphate dehydrogenase (G6PD), a genetic trait common in malaria-endemic areas. Furthermore, PQ is metabolized into carboxyprimaquine in the body, which does not have any activity against the parasite. The proposed PDC approach provides the potential to deliver PQ directly to the parasite, which could prevent its interaction with healthy tissues and slow the conversion of PQ into inactive byproducts. Further, the combination of the peptide and drug, each with distinct antiplasmodial mechanisms of action, provides the potential to avoid the formation of drug-resistant parasites. Herein, we report the design, synthesis, and biological evaluation of a library of PDIP-PQ conjugates. Various design elements of the PDCs were probed to investigate their effect on biological activity, including: (i) the location of the PDIP conjugation site, (ii) the hydrophilicity of the linker between the peptide and drug, (iii) the spacing between the peptide and drug, and (iv) whether the linker can be cleaved to release the drug cargo under conditions which mimic the intracellular environment of infected RBCs. This work demonstrates that conjugation within the flexible interhelix spacer of PDIP and incorporation of traceless cleavable linkersbearing either a disulfide or trioxolane moietyare important for maintaining the low micromolar potency of the PQ drug cargo against P. falciparum.
Click to Show/Hide
|
||||
| Description |
The six PDIP-PQ conjugates were analyzed for their ability to inhibit the in vitro growth of P. falciparum asexual blood stage parasites (strain 3D7) in RBCs and were compared to the activity of the parent drug and peptide. We were encouraged to discover that most of the PDIP-PQ PDCs retained antiplasmodial activity similar to PDIP, with IC50 values in the low micromolar range. Notably, the various design elements probed provided valuable information regarding which PDC characteristics can be modified to improve activity.
Click to Show/Hide
|
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| In Vivo Model | Plasmodium falciparum 3D7. | ||||
References