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1600418-29-8

mc-GGFG-DX is a chemical with a specific purpose. Lookchem provides you with multiple data and supplier information of this chemical.

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  • 1600418-29-8 Structure

  • Basic information

    1. Product Name: mc-GGFG-DX
    2. Synonyms:
    3. CAS NO:1600418-29-8
    4. Molecular Formula:
    5. Molecular Weight: 946.989
    6. EINECS: N/A
    7. Product Categories: N/A
    8. Mol File: 1600418-29-8.mol

  • Chemical Properties

    1. Melting Point: N/A
    2. Boiling Point: 1410.7±65.0 °C(Predicted)
    3. Flash Point: N/A
    4. Appearance: N/A
    5. Density: 1.48±0.1 g/cm3(Predicted)
    6. Refractive Index: N/A
    7. Storage Temp.: N/A
    8. Solubility: N/A
    9. CAS DataBase Reference: mc-GGFG-DX(CAS DataBase Reference)
    10. NIST Chemistry Reference: mc-GGFG-DX(1600418-29-8)
    11. EPA Substance Registry System: mc-GGFG-DX(1600418-29-8)

  • Safety Data

    1. Hazard Codes: N/A
    2. Statements: N/A
    3. Safety Statements: N/A
    4. WGK Germany:
    5. RTECS:
    6. HazardClass: N/A
    7. PackingGroup: N/A
    8. Hazardous Substances Data: 1600418-29-8(Hazardous Substances Data)

1600418-29-8 Usage

Check Digit Verification of cas no

The CAS Registry Mumber 1600418-29-8 includes 10 digits separated into 3 groups by hyphens. The first part of the number,starting from the left, has 7 digits, 1,6,0,0,4,1 and 8 respectively; the second part has 2 digits, 2 and 9 respectively.
Calculate Digit Verification of CAS Registry Number 1600418-29:
(9*1)+(8*6)+(7*0)+(6*0)+(5*4)+(4*1)+(3*8)+(2*2)+(1*9)=118
118 % 10 = 8
So 1600418-29-8 is a valid CAS Registry Number.

1600418-29-8Downstream Products

1600418-29-8Relevant articles and documents

Novel antibody drug conjugates containing exatecan derivative-based cytotoxic payloads

Nakada, Takashi,Masuda, Takeshi,Naito, Hiroyuki,Yoshida, Masao,Ashida, Shinji,Morita, Koji,Miyazaki, Hideki,Kasuya, Yuji,Ogitani, Yusuke,Yamaguchi, Junko,Abe, Yuki,Honda, Takeshi

, p. 1542 - 1545 (2016)

Trastuzumab conjugates consisting of exatecan derivatives were prepared and their biological activities and physicochemical properties were evaluated. The ADCs showed strong efficacy and a low aggregation rate. The exatecan derivatives were covalently connected via a peptidyl spacer (Gly-Gly-Phe-Gly), which is assumed to be stable in circulation, and were cleaved by lysosomal enzymes following ADC internalization into tumor tissue. These anti-HER2 ADCs exhibited a high potency, specifically against HER2-positive cancer cell lines in vitro. The ADCs, bearing exatecan derivatives which have more than two methylene chains, exhibited superior cytotoxicity. It was speculated that steric hindrance of the cleavable amide moiety could be involved in the drug release. The adequate alkyl lengths of exatecan derivatives (13, 14, 15) were from two to four in terms of aggregation rate. The ADC having a hydrophilic moiety showed good efficacy in a HER2-positive and Trastuzumab-resistant breast carcinoma cell model in mice.

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