CN2697643Y - Dissolution detector for continuously determining multi-composition medicine - Google Patents
Dissolution detector for continuously determining multi-composition medicine Download PDFInfo
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- CN2697643Y CN2697643Y CN 200320112716 CN200320112716U CN2697643Y CN 2697643 Y CN2697643 Y CN 2697643Y CN 200320112716 CN200320112716 CN 200320112716 CN 200320112716 U CN200320112716 U CN 200320112716U CN 2697643 Y CN2697643 Y CN 2697643Y
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Abstract
The utility model relates to a dissolution detector for continuously determining multi-composition medicine, belonging to the dissolution detector for continuously detecting the multi-composition medicine online. The utility model comprises a sample introducing system, an optical path system, a light splitting detection system and a computer system. The sample introducing system is composed of a sampling tube 5, a creepage pump 7, a six-channel flow pond 8, a stepped motor 9, a round bottom beaker 19, etc. The optical path system arranged on both sides of the six-channel flow pond 8 is composed of a light source, an incident optical fibre and a reflecting optical fibre. The light splitting detection system is made into a light splitting detection modular form which is the combination of a flat image field grating and an ultraviolet reinforced linear CCD array detector. The utility model with fast measurement speed reduces the hysteresis quality of the measurement, and because the CCD array detector is used, the detection of the dissolution of the multi-composition medicine can be realized. Because the modular design is adopted, the volume of the complete machine is small, and the sample introduction and the detection are all controlled by the computer. The data processing is also completed by the computer with convenient operation.
Description
Technical field
The utility model belongs to a kind of instrument of energy on-line continuous fast detecting multicomponent pharmaceutical dissolution rate.
Background technology
For a long time, in the used instrument of drug dissolution detection range, mainly be that armrest moves extracting soup from digestion instrument, after filtering, detect with ultraviolet-visible pectrophotometer.That this dissolution determination method exists is time-consuming, effort, measure shortcomings such as hysteresiss, inconvenient operation, and more owing to manual steps in measuring process, this all has relatively high expectations on professional knowledge technical ability and skill level to operating personnel.In recent years, commercial drug dissolution instrument solves these problems to a certain extent, but the ubiquity automaticity is also not high, the problem that manual operation is many.In addition, its cost is higher, thereby and not exclusively suitable developing country's medium-sized and small enterprises and institution of higher learning's use.On the other hand, this dissolution test system can not be measured the dissolution rate of multicomponent pharmaceutical simultaneously, and the exploitation of some pharmaceutical preparations has then been put on schedule to the development of the dissolution rate detector that can measure the multicomponent pharmaceutical dissolution rate simultaneously.
Up to the present, domestic dissolution rate instrument still adopts raster scanning, the method that photomultiplier detects.This raster scanning adds the pattern that photomultiplier detects, has mechanical wear on the one hand, the problem that long-time stability are unsatisfactory, measure the domestic so far patent report that does not also have the digestion instrument that can the multicomponent pharmaceutical dissolution rate detects simultaneously when it also is difficult to realize the multicomponent pharmaceutical dissolution rate on the other hand.Because this digestion instrument of development all has important directive significance for the development and the production of exploitation polycomponent, long-acting release medicine, therefore developing this detector is very to be necessary.
The utility model content
The technical problems to be solved in the utility model is: overcome existing foregoing shortcoming of current commodity drug dissolution detector and deficiency, design novel sample drawing-in system, fundamentally solved and measured the problem that lags behind, and made easy to operate, time saving and energy saving.Use the ultraviolet enhanced linear array detecting device, realized that polycomponent, multi-wavelength detect simultaneously, the problem that having solved dissolution test system now can only single wavelength, single component is measured dissolution rate.Design new spectral detection system, eliminate the mechanical wear problem that scanning mechanism exists, increase the reliability of analysis result.
The dissolution rate detector that is used for the METHOD FOR CONTINUOUS DETERMINATION multicomponent pharmaceutical of the present utility model, its structure comprise sample drawing-in system, light path system, spectral detection system, the department of computer science round bottom beaker of unifying; Said sample drawing-in system is made of stopple coupon, peristaltic pump, six passage flow cells, stepper motor, and stopple coupon inserts in the round bottom beaker and with peristaltic pump and links to each other, and peristaltic pump is connected with six passage flow cells, and six passage flow cells link to each other with stepper motor; In six passage flow cell both sides light path system is arranged, said light path system is made up of light source, convex lens, incident optical, outgoing optical fiber, and an end of incident optical and outgoing optical fiber is relative with the two ends of six passage flow cells respectively; Said spectral detection system is slit, collimation concave mirror, grating, optical convergence concave mirror and array detector by the optical propagation direction order, and the other end of outgoing optical fiber is relative with slit; Array detector is realized the electric signal input computer system after the opto-electronic conversion, and the computer system control stepper motor makes each passage two ends of six passage flow cells can pass through the incident optical of light path system and the opposite end of outgoing optical fiber successively.
Stopple coupon can be made of stainless-steel tube and thereon miillpore filter of cover, and stopple coupon directly is inserted in the soup in the dissolution rate instrument.Stopple coupon links to each other with peristaltic pump, and peristaltic pump is delivered to the soup of stopple coupon extracting in the flow cell of six passages, and six passages of flow cell come adjusting position by stepper motor.There is light path system window both sides at flow cell, and the light source in the said light path system can be a deuterium tungsten combined light source.The other end of outgoing optical fiber and the light entrance of spectral detection system, promptly slit is relative.Said spectral detection system is light entrance, parallel light concave mirror, grating, optical convergence concave mirror and CCD detecting device by the optical propagation direction order; Array detector is realized the electric signal input computer system after the opto-electronic conversion.
In the sample drawing-in system, add the stainless steel stopple coupon and on dop make stopple coupon accurately to locate, make each sample position constant, to reduce measuring error.Put miillpore filter at its end that contacts with solution, can make bulky grain be difficult to enter into flow cell, reduce scattering of light, increase the accuracy of measuring.
Six passage flow cells are Primary Components of automatic sample drawing-in system, and the profile of each passage all is opal shape, and light entrance and light exit are thinner in the passage, and channel middle is thicker.Feeder connection and outlet all are embedded with quartz window.Each channel volume has only 1mL, and sample size is little.The flow cell profile is opal shape, can reduce dead volume to greatest extent, reduces measuring error.Flow cell is fixed on the stepper motor, and stepper motor is used for regulating the position of flow cell, make six passages successively by light path system so that detect.Owing to used stepper motor, can control moving of flow cell accurately, make its accurate location, increase the reliability of measurement result.
Because the CCD linear array detecting device that the detecting device of this instrument can adopt ultraviolet to strengthen detects when can realize the multicomponent pharmaceutical dissolution rate.After the CCD detecting device is realized opto-electronic conversion, import signal into computing machine after the software processes of design voluntarily, the output data result can manifest the dissolution rate curve of different component simultaneously.Because the CCD detecting device utilizes USB interface to link to each other with computing machine, can realize plug and play, make this instrument use like this and seem convenient easy-to-use.
Spectral detection system can be made into spetroscopy detecting module form.Said beam split detection module is installed together by stationkeeping separately by parallel light concave mirror, grating, optical convergence concave mirror and array detector and constitutes; Each beam split detection module is selected the detection wavelength of different-waveband, thereby forms the beam split detection module of one group of series wavelength.During use, can pass through to change different beam split detection modules, and realize the detection of different wavelength range spectrum.Owing to adopt modular design, spectral detection system does not have movable member, change spectral range freedom, convenience, can realize that multielement (multi-wavelength) detects simultaneously, improved analysis speed, Instrument purchase and running, maintenance cost are cheap, have eliminated the mechanical wear problem that scanning mechanism exists, and have increased the reliability of analysis result.
Description of drawings
Fig. 1 is the structured flowchart that is used for the dissolution rate detector of METHOD FOR CONTINUOUS DETERMINATION multicomponent pharmaceutical of the present utility model.
Fig. 2 is a sampling system synoptic diagram of the present utility model.
Fig. 3 is a light path system synoptic diagram of the present utility model.
Fig. 4 is a spectral detection system synoptic diagram of the present utility model.
Embodiment
Below in conjunction with accompanying drawing, the concrete structure of the present utility model and the course of work are described.
Embodiment 1 the utility model is used for the one-piece construction of the dissolution rate detector of METHOD FOR CONTINUOUS DETERMINATION multicomponent pharmaceutical.
See Fig. 1, the utility model one-piece construction comprises sample drawing-in system 1, light path system 2, spectral detection system 3, computer system 4 and round bottom beaker 19.
Stopple coupon 5 extracts soup from the round bottom beaker 19 of dissolution rate instrument, the soup sample drawing-in system 1 of flowing through, the incident optical 12 of the light that light source 10 sends from light path system 2 is injected into a passage in the six passage flow cells 8 in the sample drawing-in system 1, through with flow cell 8 in the soup effect after be injected into outgoing optical fiber 13 in the light path system 2.Light penetrates after lens converge the back from outgoing optical fiber 13 and arrives spectral detection system 3, and spectral detection system 3 can adopt modular design, each parts fixed installation.After the beam split, the optical signals photoelectric coupled device is accepted, and is handled, shows, is printed by computer system 4 after opto-electronic conversion.Computer system 4 is also being controlled the work of stepper motor 9.
Embodiment 2 the utility model are used for the sample drawing-in system of the dissolution rate detector of METHOD FOR CONTINUOUS DETERMINATION multicomponent pharmaceutical.
Sample drawing-in system 1 can be made up of six stopple coupons 5, one six passage peristaltic pump 7, stepper motor 9, six passage flow cells 8.Wherein six stopple coupons 5 extract soup respectively from six round bottom beakers 19 of digestion instrument, behind peristaltic pump 7, enter into six passage flow cells, 8 corresponding passages.Moving of stepper motor 9 controls six passage flow cells 8 makes six passages pass through light path system 2 successively.Six passage principle of work of cause are just the same, the situation of only drawing one of them passage among Fig. 2.
In Fig. 2, an end has the stopple coupon 5 of miillpore filter, and its end that has a microvoid filter membrane directly contacts with soup in the round bottom beaker 19 of dissolution rate instrument, and miillpore filter can filter the bulky grain particle in the soup.The stopple coupon other end has dop 6, and dop 6 is fixed on the plexiglass cover 20 of round bottom beaker, utilizes dop 6 can make the stopple coupon spot sampling, and the end that stopple coupon has dop 6 links to each other with peristaltic pump 7.Peristaltic pump 7 is power resources of sample drawing-in system 1, and peristaltic pump 7 is incorporated into a passage in the six passage flow cells 8 with soup, and the back soup flow back in the round bottom beaker 19 of dissolution rate instrument after testing.
Embodiment 3 light path systems that are used for the dissolution rate detector of METHOD FOR CONTINUOUS DETERMINATION multicomponent pharmaceutical of the present utility model.
See Fig. 3, the light path system 2 that is used for the dissolution rate detector of METHOD FOR CONTINUOUS DETERMINATION multicomponent pharmaceutical is made up of light source 10, convex lens 11, incident optical 12, outgoing optical fiber 13.The light that light source 10 sends enters into incident optical 12 after being assembled by convex lens 11, is injected into a passage in the six passage flow cells then.After the soup effect in light and the passage, be injected into outgoing optical fiber 13, derive in order to detecting by outgoing optical fiber 13 then.
Embodiment 4 the utility model are used for the spectral detection system of the dissolution rate detector of METHOD FOR CONTINUOUS DETERMINATION multicomponent pharmaceutical.
See Fig. 4,18 is light entrance, corresponding with an end of outgoing optical fiber 13; 14 is the parallel light concave mirror, fiber optic line is gone into the light that oral instructions come be reflected into directional light, shines on the grating 15 again, and grating 15 can be the flat field grating; Here complex light through projecting on the ultraviolet enhanced linear array detecting device 17 behind the optical convergence concave mirror 16, is realized the opto-electronic conversion of whole wavelength coverage by the monochromatic light of grating 15 chromatic dispersions one-tenth according to Wavelength distribution.Electric signal after the conversion is finished multi-component measurement simultaneously in the sample solution by demonstration and the print system demonstration and the printing of computing machine 4 controls.Using ultraviolet enhanced linear array detecting device 17 is the keys that realize that medicine polycomponent dissolution rate is measured.
Claims (3)
1, a kind of dissolution rate detector that is used for the METHOD FOR CONTINUOUS DETERMINATION multicomponent pharmaceutical, its structure comprises sample drawing-in system (1), light path system (2), spectral detection system (3), computer system (4) and round bottom beaker (19); It is characterized in that, said sample drawing-in system is made of stopple coupon (5), peristaltic pump (7), six passage flow cells (8), stepper motor (9), stopple coupon (5) inserts in the round bottom beaker (19) and with peristaltic pump (7) and links to each other, peristaltic pump (7) is connected with six passage flow cells (8), and six passage flow cells (8) link to each other with stepper motor (9); In six passage flow cell (8) both sides light path system (2) is arranged, said light path system (2) is made up of light source (10), convex lens (11), incident optical (12), outgoing optical fiber (13), and an end of incident optical (12) and outgoing optical fiber (13) is relative with the two ends of six passage flow cells (8) respectively; Said spectral detection system (3) is slit (18), collimation concave mirror (14), grating (15), optical convergence concave mirror (16) and array detector (17) by the optical propagation direction order, and the other end of outgoing optical fiber (13) is relative with slit (18); Array detector (17) is realized the electric signal input computer system (5) after the opto-electronic conversion, computer system (4) control step motor (9) make six each passage two ends of passage flow cell (8) can be successively the opposite end of incident optical (12) and outgoing optical fiber (13) by light path system.
2, according to the described dissolution rate detector that is used for the METHOD FOR CONTINUOUS DETERMINATION multicomponent pharmaceutical of claim 1, it is characterized in that, said stopple coupon (5), the one end is with miillpore filter, the other end links to each other with dop (6), and the organic glass that dop (6) is fixed on digestion instrument round bottom beaker (19) covers (20); Said six each passage of passage flow cell (8) are opal shape; Said stepper motor (9) is secured together with six passage flow cells (8).
According to claim 1 or the 2 described dissolution rate detectors that are used for the METHOD FOR CONTINUOUS DETERMINATION multicomponent pharmaceutical, it is characterized in that 3, spectral detection system (4) adopts flat field grating and ultraviolet to strengthen array detector and matches, promptly said grating (15) is the flat field grating; Said array detector (17) is that ultraviolet strengthens array detector; Spectral detection system (4) is made into the form of beam split detection module, said beam split detection module by collimation concave mirror (14), grating (15), optical convergence concave mirror (16) and array detector (17) by the light path formation that is fixedly installed togather, the detection wavelength of each beam split detection module selection different-waveband.
Priority Applications (1)
| Application Number | Priority Date | Filing Date | Title |
|---|---|---|---|
| CN 200320112716 CN2697643Y (en) | 2003-11-13 | 2003-11-13 | Dissolution detector for continuously determining multi-composition medicine |
Applications Claiming Priority (1)
| Application Number | Priority Date | Filing Date | Title |
|---|---|---|---|
| CN 200320112716 CN2697643Y (en) | 2003-11-13 | 2003-11-13 | Dissolution detector for continuously determining multi-composition medicine |
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| Publication Number | Publication Date |
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| CN2697643Y true CN2697643Y (en) | 2005-05-04 |
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| CN 200320112716 Expired - Fee Related CN2697643Y (en) | 2003-11-13 | 2003-11-13 | Dissolution detector for continuously determining multi-composition medicine |
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Cited By (4)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| CN100456019C (en) * | 2003-11-13 | 2009-01-28 | 吉林大学 | Dissolving degree detector for continuously detecting multiple component medicine |
| CN103048161A (en) * | 2011-10-15 | 2013-04-17 | 四川汇利实业有限公司 | Sampling pipe convenient to hold for dissolution instrument |
| CN103076296A (en) * | 2010-03-16 | 2013-05-01 | 新疆富科思生物技术发展有限公司 | Background interference elimination method for UV visible absorption spectrum of optical fiber in situ drug dissolution/releasing rate tester |
| CN105043999A (en) * | 2015-06-09 | 2015-11-11 | 中国中医科学院中药研究所 | Method for determining dissolution rate of medicinal preparation containing salvianolic acid components |
-
2003
- 2003-11-13 CN CN 200320112716 patent/CN2697643Y/en not_active Expired - Fee Related
Cited By (6)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| CN100456019C (en) * | 2003-11-13 | 2009-01-28 | 吉林大学 | Dissolving degree detector for continuously detecting multiple component medicine |
| CN103076296A (en) * | 2010-03-16 | 2013-05-01 | 新疆富科思生物技术发展有限公司 | Background interference elimination method for UV visible absorption spectrum of optical fiber in situ drug dissolution/releasing rate tester |
| CN103076296B (en) * | 2010-03-16 | 2015-03-11 | 新疆富科思生物技术发展有限公司 | Background interference elimination method for UV visible absorption spectrum of optical fiber in situ drug dissolution/releasing rate tester |
| CN103048161A (en) * | 2011-10-15 | 2013-04-17 | 四川汇利实业有限公司 | Sampling pipe convenient to hold for dissolution instrument |
| CN105043999A (en) * | 2015-06-09 | 2015-11-11 | 中国中医科学院中药研究所 | Method for determining dissolution rate of medicinal preparation containing salvianolic acid components |
| CN105043999B (en) * | 2015-06-09 | 2018-02-06 | 中国中医科学院中药研究所 | A kind of dissolution determination method of the pharmaceutical preparation containing salvianolic acid component |
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| C14 | Grant of patent or utility model | ||
| GR01 | Patent grant | ||
| C19 | Lapse of patent right due to non-payment of the annual fee | ||
| CF01 | Termination of patent right due to non-payment of annual fee |