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Micro fluidic chip device for combined detection of six typical tumor markers

A technology of microfluidic chips and tumor markers, which is applied in the field of microfluidic chip devices, can solve the problems that the fine liquid flow is difficult to pass, has not been properly solved, and the operation of modifying the inner surface of PDMS microchannels is troublesome.

Inactive Publication Date: 2018-02-16
洪小女
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  • Summary
  • Abstract
  • Description
  • Claims
  • Application Information

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Problems solved by technology

[0008] But it's not that simple
[0009] First, this polydimethylsiloxane material, the material referred to by the acronym PDMS, is itself a strongly hydrophobic material. Microchannels are built on this material. If the microchannels are not targeted The modification operation of the surface of the channel, then, after the overall assembly is completed, that is, after the cover is covered, because the inner surface of the micro channel in the structure occupies most of the inner surface of the liquid flow channel, then the PDMS micro channel The strong hydrophobic characteristic of the inner surface of the channel is the decisive factor, which will make it very difficult for the polar liquid flow similar to the aqueous solution to pass through, and its flow resistance is so large that even ordinary micropumps are difficult to push. Of course, If the cover sheet also chooses to use the PDMS material, then the problem is basically the same, with little difference; therefore, in the prior art, it is necessary to modify and modify the inner surface of the microchannel on the PDMS material; then , is this modification operation for the inner surface of the PDMS microchannel very troublesome? That's not the problem. What constitutes a serious technical problem is another problem: the PDMS polymer molecules in the bulk phase of the PDMS material substrate have the characteristics of automatic diffusion and migration to the surface. The characteristics of polymer molecules diffusing and migrating to the surface automatically will make the modified state of the inner surface of the microchannel modified by the surface modification unable to maintain for a long enough time, and the microgroove after surface modification The maintenance time of the inner surface state of the channel is roughly only enough to complete the time required for the internal test experiment in the laboratory; in other words, the inner surface of the PDMS microchannel after surface modification or surface modification is formed after modification The surface state of the surface does not last long, but quickly tends to or changes back to the surface state before the surface modification, and returns to the original strongly hydrophobic surface state in a relatively short period of time. Then, just imagine, Can such microfluidic chips be produced in large quantities, stored in large quantities, and widely promoted? The answer is obvious, that is, impossible
This problem has also existed for many years, and so far, it has not been properly solved

Method used

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  • Micro fluidic chip device for combined detection of six typical tumor markers

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Embodiment Construction

[0059] in figure 1 In the example shown in this case, the main point of this example is that the structure of the device includes a multi-channel microfluidic chip, and the structure of the microfluidic chip includes a substrate 5 and a cover sheet 6 that are attached to each other. The substrate 5 and the cover sheet 6 are both plate-like or sheet-like objects, and the surface of the substrate 5 facing the cover sheet 6 contains a channel structure formed by a molding process or an etching process. 5 also contains a window structure that is connected to the channel structure and penetrates the substrate 5 and is formed through a molding process, an etching process or a simple perforation process. The substrate 5 and the cover sheet 6 are attached to each other and are mounted together. Constructed into a microfluidic chip containing a pipe structure and a liquid pool structure connected to it. The pipe structure is located at the interface area where the substrate 5 and the co...

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Abstract

The invention relates to a microfluidic chip device for combined detection of six typical tumor markers, belonging to the field of analysis and testing. Polydimethylsiloxane, or PDMS, is used to make the substrate of a microfluidic chip for multi-channel combined detection of typical tumor markers. It has advantages and problems; this case addresses this problem. The main point of this case is that the PDMS with the original ecological surface is selected as the substrate, and the elastic clamp with the micro-ultrasonic transducer attached to the clamping arm is elastically positioned on the sample liquid flow terminal of the microfluidic chip and its neighbors. position, using ultrasonic waves to reduce the interfacial tension, greatly increasing the interfacial compatibility between the solid and liquid phases, and at the same time using the strong absorption capacity of PDMS for ultrasonic waves, the intensity of ultrasonic waves decreases rapidly within a short distance, thus forming at both ends of the chip The difference in interfacial tension thereby facilitates the flow of the sample fluid toward the terminal along the originally strongly hydrophobic capillary channel. The device eliminates the need for a micropump.

Description

Technical field [0001] The invention relates to a microfluidic chip device for combined detection of typical six tumor markers, belonging to the field of analysis and testing. Background technique [0002] Tumor marker (TM) refers to a class of substances that are produced by tumor cells themselves or by the body’s response to tumor cells during the occurrence and proliferation of tumors, and reflect the existence and growth of tumors, including Proteins, hormones, enzymes (isoenzymes) and oncogene products, etc. Testing the tumor markers in the blood or body fluid of the patient can detect the tumor early in the tumor screening, and observe the efficacy of tumor treatment and judge the prognosis of the patient. Currently commonly used clinical tumor markers are: (1) alpha-fetoprotein (AFP) is a marker for primary liver cancer, testicular cancer, ovarian cancer and other tumors; (2) carcinoembryonic antigen (CEA) is a tumor of the digestive system, Markers for lung cancer, brea...

Claims

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Application Information

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IPC IPC(8): B01L3/00G01N33/574
CPCB01L3/5027B01L3/50273B01L2200/10B01L2300/0861B01L2300/0887B01L2300/12B01L2300/161B01L2400/0439B01L2400/0475G01N33/57484
Inventor 洪小女
Owner 洪小女
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