The development of orally administrable gemcitabine prodrugs with D-enantiomer amino acids: enhanced membrane permeability and enzymatic stability - Wikidata - awgldk - TriplyDB

The development of orally administrable gemcitabine prodrugs with D-enantiomer amino acids: enhanced membrane permeability and enzymatic stability

The development of orally administrable gemcitabine prodrugs with D-enantiomer amino acids: enhanced membrane permeability and enzymatic stability

http://www.wikidata.org/entity/Q34570055

about

Amino Acid Derivatives as Palmitoylethanolamide Prodrugs: Synthesis, In Vitro Metabolism and In Vivo Plasma Profile in Rats Eradication of Enterococcus faecalis Biofilms on Human Dentin.Pancreatic Cancer Chemoresistance to Gemcitabine.On the design principles of peptide-drug conjugates for targeted drug delivery to the malignant tumor site.Encapsulating a Hydrophilic Chemotherapeutic into Rod-like Nanoparticles of a Genetically Encoded Asymmetric Triblock Polypeptide Improves its Efficacy Amino Acids in the Development of Prodrugs Thymoquinone synergizes gemcitabine anti-breast cancer activity via modulating its apoptotic and autophagic activities

P2860

Q28548007-B5041AB1-5363-42B5-AB19-EFB409A31FF2 Q39827388-7D0EF85F-6088-4A11-A36A-12CDE53ABEA5 Q47135556-4183F89E-9D6E-4BBD-B1F3-17D672D49300 Q55054276-7736ADCA-D6F9-4516-8926-8CDBB6BBCCE0 Q57498771-1BA132DA-BB49-4902-9B23-DFA65FA759D2 Q58696356-CA770E7F-5AE0-47A4-A096-9C3F426B83AA Q58802359-B9AC5F51-EDC7-4CFA-8714-091923DB4103

P2860

The development of orally administrable gemcitabine prodrugs with D-enantiomer amino acids: enhanced membrane permeability and enzymatic stability

http://www.wikidata.org/entity/Q34570055

description

2013 nî lūn-bûn

@nan

2013 թուականի Դեկտեմբերին հրատարակուած գիտական յօդուած

@hyw

2013 թվականի դեկտեմբերին հրատարակված գիտական հոդված

@hy

2013年の論文

@ja

2013年論文

@yue

2013年論文

@zh-hant

2013年論文

@zh-hk

2013年論文

@zh-mo

2013年論文

@zh-tw

2013年论文

@wuu

name

The development of orally admi ...... bility and enzymatic stability

@ast

The development of orally admi ...... bility and enzymatic stability

@en

The development of orally admi ...... bility and enzymatic stability

@nl

type

label

The development of orally admi ...... bility and enzymatic stability

@ast

The development of orally admi ...... bility and enzymatic stability

@en

The development of orally admi ...... bility and enzymatic stability

@nl

prefLabel

The development of orally admi ...... bility and enzymatic stability

@ast

The development of orally admi ...... bility and enzymatic stability

@en

The development of orally admi ...... bility and enzymatic stability

@nl

P1433

Q34570055-D63DDDEE-020F-4636-AFD8-17E129AC986C

P1476

Q34570055-9C67E255-5A7F-442E-85D0-9C2F6228FFF0

P2093

Q34570055-199C5D05-11C2-49F7-854A-5ACD5929321F

Q34570055-74ACDFA5-7656-4656-9685-73F5C4E17846

Q34570055-78B0AD91-C229-4A85-806E-A304D3BD4EB2

Q34570055-FABD2CCF-9732-4F39-A72A-102A13651778

P2860

Q34570055-05DF9FCA-2BAE-4CEE-AA16-C709E800C118

Q34570055-0CE60847-F7A0-40D2-A873-E39F09596AC1

Q34570055-18980BFB-9683-4690-80D7-FEC09758720D

Q34570055-1A69780D-7054-4340-A438-B0E50DACAA44

Q34570055-1D8FE8AA-E979-4C17-B541-4DDC987AADC3

Q34570055-1EDFB9C7-4288-4AE2-9542-28D3C79A9A72

Q34570055-323F0F33-FF21-4012-9AA4-21FE30FEE66A

Q34570055-37541200-8383-4E52-AEB9-A27954EA3E1F

Q34570055-4763BB5E-C4C4-4EB7-ABC2-053335BAB3E0

Q34570055-4CBB93C4-0AA4-439A-B1B6-832287ACAED1

P304

Q34570055-80AEF878-023D-4FD6-844B-9F480EC73043

P31

Q34570055-A4C515FE-A095-431A-A5CE-631EADCDE598

P356

Q34570055-275B0122-281D-49DE-ACEE-CBE2B3C66CCF

P407

Q34570055-FC27D5E2-88BD-4638-8CB8-5719C698B6CC

P433

Q34570055-2E56C3B0-E6A9-4E45-B889-9E666E9B1F82

P478

Q34570055-3F09F6FB-2FF5-4E5B-BB96-4FF91EFD2A07

P50

Q34570055-0A2E8FDA-9885-443C-B264-96CDBB4263E3

P577

Q34570055-A1FFA7CA-42E7-4332-AE20-C4F02AD87764

P698

Q34570055-F0D88776-C54C-4BD5-9883-1187AEBE50FB

P932

Q34570055-B9D166A2-5CC3-48C7-9890-BD3B84F99731

P356

J.EJPB.2013.12.009

P1433

European Journal of Pharmaceutics and Biopharmaceutics

P1476

The development of orally admi ...... bility and enzymatic stability

@en

P2093

Gordon L Amidon

http://www.w3.org/2001/XMLSchema#string

John M Hilfinger

http://www.w3.org/2001/XMLSchema#string

Xueqin Song

http://www.w3.org/2001/XMLSchema#string

Yasuhiro Tsume

http://www.w3.org/2001/XMLSchema#string

P2860

Algorithmic modeling quantifies the complementary contribution of metabolic inhibitions to gemcitabine efficacy

Mammalian peptide transporters as targets for drug delivery.

hPEPT1 affinity and translocation of selected Gln-Sar and Glu-Sar dipeptide derivatives.

Bioavailability of aciclovir after oral administration of aciclovir and its prodrug valaciclovir to patients with leukopenia after chemotherapy

5-Fluorouracil: forty-plus and still ticking. A review of its preclinical and clinical development.

Metastatic breast cancer: we do need primary cost data.

Nucleoside transporter profiles in human pancreatic cancer cells: role of hCNT1 in 2',2'-difluorodeoxycytidine- induced cytotoxicity.

An oligopeptide transporter is expressed at high levels in the pancreatic carcinoma cell lines AsPc-1 and Capan-2.

Pharmacokinetics of the acyclovir pro-drug valaciclovir after escalating single- and multiple-dose administration to normal volunteers.

Current prodrug strategies via membrane transporters/receptors.

P304

514-523

http://www.w3.org/2001/XMLSchema#string

P31

scholarly article

P356

10.1016/J.EJPB.2013.12.009

http://www.w3.org/2001/XMLSchema#string

P407

P433

3

http://www.w3.org/2001/XMLSchema#string

P478

86

http://www.w3.org/2001/XMLSchema#string

P50

P577

2013-12-19T00:00:00Z

http://www.w3.org/2001/XMLSchema#dateTime

P698

24361461

http://www.w3.org/2001/XMLSchema#string

P932

4243704

http://www.w3.org/2001/XMLSchema#string