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首頁 > PNA定制合成 > PNA Clamp Kit
PNA 合成
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多肽合成
PNA Clamp Kit
  • PNAClamp 技術(shù)是指PNA能夠?qū)R恍缘呐c野生型DNA結(jié)合,從而使野生型DNA不能作為模板進(jìn)行PCR擴(kuò)增;而突變型DNA,由于堿基的缺失或突變,PNA不能與其結(jié)合,從而使突變型DNA能夠進(jìn)行PCR擴(kuò)增。

    一般來說,一個樣本中,大部分是野生型DNA,突變型DNA只占極少的一部分,因此通過一般的PCR很難檢測到突變型DNA的存在。如果在樣本中加入與野生型DNA互補(bǔ)的PNA,則野生型DNA與PNA牢固結(jié)合,使得野生型DNA不能進(jìn)行PCR擴(kuò)增,由于沒有野生型DNA的干擾,突變性DNA能夠很容易被擴(kuò)增并檢測。


    PNAClamp Mutation detection 的原理:

    1. 與 DNA/DNA 的結(jié)合相比,在不存在錯配的情況下,PNA/DNA 的結(jié)合穩(wěn)定性更強(qiáng)(每增加 1 base 序列,退火溫度增加 ~1℃)。

    2. 與 DNA/DNA 的結(jié)合相比,在存在錯配的情況下,PNA/DNA 的結(jié)合穩(wěn)定性更差。

    3. PNA 不能作為引物被 DNA polymerase 識別并擴(kuò)增。


    PNAClamp Mutation detection Kits 的優(yōu)勢:

    1. 檢測時間短(約2小時)。

    2. 操作簡單。

    3. 需要樣品少(低至1~25ng DNA樣品)。

    4. 靈敏度高。

    5. 穩(wěn)定性強(qiáng)。

    6. 保質(zhì)期長。

    7. 可以在多種型號的熒光定量PCR儀中使用(如:BI-7500, ABI-7900HT, Biorad CFX-96/384, Roche Lightcycler, Qiagen RGQ etc)。

    8. 數(shù)據(jù)分析簡單明了。


    PNAClamp Mutation detection 示意圖:




  •    The epidermal growth factor receptor (EGFR) is a family member of Receptor tyrosine kinases, expressed on the surface of epidermal cells. Overexpression or overactivation of EGFR is linked to a number of cancers, including lung cancer, anal cancers and glioblastoma multiform.

       The PNAClamp EGFR Mutation Detection Kit detects most prevalent mutations described to date in the EGFR gene, including T790M, the presence of which correlates with resistance to tyrosine kinase inhibitors. Detecting somatic mutations in EGFR gene may provide a useful strategy to predict the response to the tyrosine kinase inhibitors in efforts to increase the survival rate of lung cancer patients receiving targeted therapy.


    Exon

    Amino acid change

    Base change

    18

    Gly719Ala

    2156 G>C

    Gly719Ser

    2155 G>A

    Gly719Cys

    2155 G>T

    19

    Glu746_Ala750del

    2235_2249 del 15

    Glu746_Thr751delinslle

    2235_2252 AAT (complex)

    Glu746_Ser752del

    2236_2253 del 18

    Glu746_Thr751delinsAla

    2237_2251 del 15

    E746_S752>A

    2237_2254 del 18

    Glu746_Ser752delinsVal

    2237_2255 >T (complex)

    Glu746_Ala750del

    2236_2250 del 15

    Glu746_Ser752delinsAsp

    2238_2255 del 18

    L747_A750>P

    2238_2248 >GC (complex)

    Leu747_Thr751delinsGln

    2238_2252 >GCA (complex)

    Leu747_Glu749del

    2239_2247 del 9

    Leu747_Thr751del

    2239_2253 del 15

    Leu747_Ser752del

    2239_2256 del 18

    Leu747_Glu749del:Ala750Pro

    2239_2248 TTAAGAGAAG>C

    Leu747_Pro753delinsGln

    2239_2258 >CA (complex)

    Leu747_Thr751delinsSer

    2240_2251 del 12

    Leu747_Pro753delinsSer

    2240_2257 del 18

    Leu747_Thr751del

    2240_2254 del 15

    Leu747_Thr751deinsPro

    2239_2251 >C (complex)

    20

    Thr790Met

    2369 C>T

    Ser768lle

    2303 G>T

    Ala767_Val769dupAlaSerVal

    2307_2308 ins9

    His773dupHis

    2319_2320 insCAC

    Asp770_A771insGly

    2310_2311 insGGT

    21

    leu858Arg

    2573 T>G

    leu861Gln

    2582 T>A

  • KRAS mutation is found in several cancers including colorectal, lung, thyroid, and pancreatic cancers and cholangiocarcinoma. KRAS mutations are often located within codons 12 and 13 of exon 2, which may lead to abnormal growth signaling by the p21-ras protein. These alterations in cell growth and division may trigger cancer development as signaling is excessive.

    A KRAS mutation often serves as a useful prognostic marker of drug response. For example, a KRAS mutation is considered to be a strong prognostic marker of response to tyrosine kinase inhibitors such as gefitinib (Iressa) or erlotinib (Tarceva). Recently, KRAS mutations have been detected in many colorectal cancer patients and may be associated with responses to cetuximab (Erbitux) or panitumumab (Vectibix), which are used in colon cancer therapy.



    Codon

    Mutation

    Base change

    Codon12

    Gly12Asp

    35G>A

    Gly12Ala

    35G>C

    Gly12Val

    35G>T

    Gly12Ser

    34G>A

    Gly12Arg

    34G>C

    Gly12Cys

    34G>T

    Codon13

    Gly13Ser

    34G>T

    Gly13Arg

    37G>C

    Gly13Cys

    37G>T

    Gly13Asp

    38G>A

    Gly13Ala

    38G>C

    Gly13Val

    38G>T

    Codon59

    Ala59Ser

    175G>T

    Ala59Thr

    175GA

    Ala59Glu

    176C>A

    Ala59Gly

    176C>G

    Ala59del

    176_178 del CAG

    Codon61

    Gly60Asp

    179G>A

    Gly60Ala

    179G>C

    Gly60Val

    179G>T

    Gly60Gly

    180T>A

    Gly60Gly

    180T>C

    Gln61Glu

    181C>G

    Gln61Lys

    181C>A

    Gln61Leu

    182A>T

    Gln61Arg

    182A>G

    Gln61Pro

    182A>C

    Gln61His

    183A>T

    Gln61His

    183A>C

    Codon 117

    Lys117Glu

    349A>G

    Lys117Arg

    350A>G

    Lys117Asn

    351A>C

    Lys117Asn

    351A>T

    Codon 146

    Ala146Pro

    436G>C

    Ala146Thr

    436G>A

    Ala146Gly

    437C>G

    Ala146Val

    437C>T

    Ala146Ala

    438A>G

    Ala146Ala

    438A>C

    Ala146Ala

    438A>T



  •      PI3K (Phosphoinositide 3-kinases or PI 3-Kinases) are family of lipid kinases capable of phosphorylating the 3' position hydroxyl group of the inositol ring of phosphatidylinositol. They are involved in coordinating a diverse range of cell functions including cell growth, proliferation, differentiation, motility, survival and intracellular trafficking.

         Activating mutations in PI3K catalytic domain of the p110alpha subunit (PIK3CA) have recently been discovered in certain types of cancer cells. PIK3CA mutations are found at 25~40 % frequency in various types of tumors including colorectal cancer, gastric cancer, lung cancer, brain cancer, endometrial cancer, ovarian cancer, breast cancer. About 80% of the point mutations presides in exon 9 (a presumed helical domain) and exon 20 (a presumed kinase domain), while other types of mutations are also seen in different locations.






    Tube No

    Reagent

    Amino Acid Change

    Base change

    Exon

    Translation region

    1

    E542

    Glu542Lys

    1624 G>A

    Exon 9

    Helical

    Glu542Gly

    1624 A>G

    Glu542Val

    1624 A>T

    2

    E545

    Glu545Lys

    1633 G>A

    Glu545Gly

    1634 A>G

    Glu545Asp

    1635 G>T

    3

    H1047

    His1047Tyr

    3139 C>T

    Exon 20

    Kinase

    His1047Leu

    3140 A>T

    His1047Arg

    3140 A>G

  • 產(chǎn)品信息:


    Catalog No.

    Product Name

    Description

    Size

    Price

    PNAC-1002

    PNAClamp KRAS Kit (v2)

    G12, G13

    30 tests

    Inquire

    PNAC-1003

    PNAClamp KRAS Kit (v3)

    G12, G13, Q61

    25 tests

    Inquire

    PNAC-1004

    PNAClamp KRAS Kit (plus)

    A59, K117, A146

    25 tests

    Inquire

    PNAC-1006

    PNAClamp KRAS Kit (v4)

    G12, G13, A59, Q61, K117, A146

    25 tests

    Inquire

    PNAC-1101

    PNAClamp NRAS Kit (v4)

    G12, G13, A59, Q61, K117, A146

    25 tests

    Inquire

    PNAC-2001

    PNAClamp BRAF Kit

    BRAF V600 mutation

    50 tests

    Inquire

    PNAC-3002

    PNAClamp EGFR Kit

    G619, E19 del, T790, S768, E20 in, L858, L861

    25 tests

    Inquire

    PNAC-4002

    PNAClamp PIK3CA Kit

    E542, E545, H1047

    25 tests

    Inquire

    PNAC-5001

    PNAClamp IDH1 Kit

    R132 mutation

    25 tests

    Inquire

PNA 產(chǎn)品
多肽合成
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