Resistance mutation info of drug

Drug General Information

Drug ID

D03EDQ

Drug Name

Vismodegib

Synonyms

879085-55-9; GDC-0449; Erivedge; 2-chloro-N-(4-chloro-3-(pyridin-2-yl)phenyl)-4-(methylsulfonyl)benzamide; Vismodegib (GDC-0449); HhAntag691; GDC0449; GDC 0449; UNII-25X868M3DS; CHEMBL473417; CHEBI:66903; 25X868M3DS; NSC755986; AK-77261; 2-chloro-N-[4-chloro-3-(pyridin-2-yl)phenyl]-4-(methylsulfonyl)benzamide; C19H14Cl2N2O3S; 2-chloro-N-(4-chloro-3-pyridin-2-ylphenyl)-4-methylsulfonylbenzamide; 2-chloro-n-(4-chloro-3-(2-pyridinyl)phenyl)-4-(methylsulfonyl)benzamide; Erivedge (TN); Vismodegib (SHH inhibitor); Gdc-0449

Drug Type

Small molecular drug

Company

Genentech

Structure

Drug Resistance Mutations

Target Name

Smoothened homolog (SMO)

Target Info

Gene Name

SMO

Uniprot ID

SMO_HUMAN

Species

Homo sapiens

Reference Sequence

MAAARPARGPELPLLGLLLLLLLGDPGRGAASSGNATGPGPRSAGGSARRSAAVTGPPPP
LSHCGRAAPCEPLRYNVCLGSVLPYGATSTLLAGDSDSQEEAHGKLVLWSGLRNAPRCWA
VIQPLLCAVYMPKCENDRVELPSRTLCQATRGPCAIVERERGWPDFLRCTPDRFPEGCTN
EVQNIKFNSSGQCEVPLVRTDNPKSWYEDVEGCGIQCQNPLFTEAEHQDMHSYIAAFGAV
TGLCTLFTLATFVADWRNSNRYPAVILFYVNACFFVGSIGWLAQFMDGARREIVCRADGT
MRLGEPTSNETLSCVIIFVIVYYALMAGVVWFVVLTYAWHTSFKALGTTYQPLSGKTSYF
HLLTWSLPFVLTVAILAVAQVDGDSVSGICFVGYKNYRYRAGFVLAPIGLVLIVGGYFLI
RGVMTLFSIKSNHPGLLSEKAASKINETMLRLGIFGFLAFGFVLITFSCHFYDFFNQAEW
ERSFRDYVLCQANVTIGLPTKQPIPDCEIKNRPSLLVEKINLFAMFGTGIAMSTWVWTKA
TLLIWRRTWCRLTGQSDDEPKRIKKSKMIAKAFSKRHELLQNPGQELSFSMHTVSHDGPV
AGLAFDLNEPSADVSSAWAQHVTKMVARRGAILPQDISVTPVATPVPPEEQANLWLVEAE
ISPELQKRLGRKKKRRKRKKEVCPLAPPPELHPPAPAPSTIPRLPQLPRQKCLVAAGAWG
AGDSCRQGAWTLVSNPFCPEPSPPQDPFLPSAPAPVAWAHGRRQGLGPIHSRTNLMDTEL
MDADSDF [Homo sapiens]

Targeted Disease

Medulloblastoma

Drug Resistance Mutations

Mutation info	Missense: D473H				[1]

Mutation info	Missense: D473G				[2], [3]
Mutation Frequency	6 out of 14 patients

Mutation info	Missense: L412F				[2], [3]

Mutation info	Missense: Q477E				[2], [3]
Mutation Frequency	1 out of 30 patients

Mutation info	Missense: W281C				[2], [3]
Mutation Frequency	2 out of 30 patients

Mutation info	Missense: W535L				[2], [3]
Mutation Frequency	4 out of 30 patients

Mutation info	Missense: V321M				[4], [5]
Mutation Frequency	2 out of 12 patients

Mutation info	Missense: G497W				[2], [3]

Mutation info	Missense: W281L				[4]

Mutation info	Missense: D473Y				[2]

Mutation info	Missense: A459V				[5]
Mutation Frequency	3 out of 12 patients

Mutation info	Missense: C469Y				[5]
Mutation Frequency	1 out of 12 patients

Mutation info	Missense: T241M				[5]
Mutation Frequency	1 out of 12 patients

Mutation info	Missense: D473N				[3]
Mutation Frequency	1 out of 30 patients

Mutation info	Missense: F460L				[3]
Mutation Frequency	1 out of 30 patients

Mutation info	Missense: H231R				[3]
Mutation Frequency	2 out of 30 patients

Mutation info	Missense: S533N				[3]

Mutation info	Missense: V321A				[3]
Mutation Frequency	1 out of 30 patients

Mutation info	Missense: W535R				[3]
Mutation Frequency	4 out of 30 patients

Mutation info	Missense: D473H				[1]

Mutation info	Missense: D473G				[2], [3]
Mutation Frequency	6 out of 14 patients

Mutation info	Missense: L412F				[2], [3]

Mutation info	Missense: Q477E				[2], [3]
Mutation Frequency	1 out of 30 patients

Mutation info	Missense: W281C				[2], [3]
Mutation Frequency	2 out of 30 patients

Mutation info	Missense: W535L				[2], [3]
Mutation Frequency	4 out of 30 patients

Mutation info	Missense: V321M				[4], [5]
Mutation Frequency	2 out of 12 patients

Mutation info	Missense: G497W				[2], [3]

Mutation info	Missense: W281L				[4]

Mutation info	Missense: D473Y				[2]

Mutation info	Missense: A459V				[5]
Mutation Frequency	3 out of 12 patients

Mutation info	Missense: C469Y				[5]
Mutation Frequency	1 out of 12 patients

Mutation info	Missense: T241M				[5]
Mutation Frequency	1 out of 12 patients

Mutation info	Missense: D473N				[3]
Mutation Frequency	1 out of 30 patients

Mutation info	Missense: F460L				[3]
Mutation Frequency	1 out of 30 patients

Mutation info	Missense: H231R				[3]
Mutation Frequency	2 out of 30 patients

Mutation info	Missense: S533N				[3]

Mutation info	Missense: V321A				[3]
Mutation Frequency	1 out of 30 patients

Mutation info	Missense: W535R				[3]
Mutation Frequency	4 out of 30 patients

References

REF 1

Smoothened mutation confers resistance to a Hedgehog pathway inhibitor in medulloblastoma. Science. 2009 Oct 23;326(5952):572-4.

REF 2

Smoothened (SMO) receptor mutations dictate resistance to vismodegib in basal cell carcinoma. Mol Oncol. 2015 Feb;9(2):389-97.

REF 3

Smoothened variants explain the majority of drug resistance in basal cell carcinoma. Cancer Cell. 2015 Mar 9;27(3):342-53.

REF 4

Acquired resistance to the Hedgehog pathway inhibitor vismodegib due to smoothened mutations in treatment of locally advanced basal cell carcinoma. J Am Acad Dermatol. 2014 Nov;71(5):1005-8.

REF 5

Genomic analysis of smoothened inhibitor resistance in basal cell carcinoma. Cancer Cell. 2015 Mar 9;27(3):327-41.

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