CN201618442U - Three-band analogue moving bed chromatogram device - Google Patents
Three-band analogue moving bed chromatogram device Download PDFInfo
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- CN201618442U CN201618442U CN 200920277023 CN200920277023U CN201618442U CN 201618442 U CN201618442 U CN 201618442U CN 200920277023 CN200920277023 CN 200920277023 CN 200920277023 U CN200920277023 U CN 200920277023U CN 201618442 U CN201618442 U CN 201618442U
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Abstract
The utility model discloses a three-band analogue moving bed chromatogram device which comprises N chromatographic columns, two eluant transfer pumps, a feeding liquid delivering pump, 6N automatic control valves, a PLC or single chip machine automatic control system, a multi-way, a pipeline and a liquid storing tank, wherein N is greater than or equal to 3, but smaller than or equal to 24. The flowing phase inlet of each chromatographic column is divided into four passages by the multi-way Ii, the eluant P, the eluant D, the raw material liquid F and the previous chromatographic column circulating liquid are led into the four passages, and the four passages are controlled by the automatic control valves Pi, Di, Fi and Ti-1. The first chromatographic column is connected with the Nth chromatographic column through the automatic control valve in an end-to-end way. The flowing phase inlet of each chromatographic column is divided into three passages by the multi-way Ii, the raffinate liquid R, the extracting liquid E and the current chromatographic column circulating liquid are outputted, and the three passages are controlled by the automatic control valves Ri, Ei and Ti, so the three-band analogue moving bed chromatogram running mode with independent I band or the three-band analogue moving bed chromatogram running mode with reflux between bands I-II is formed. The utility model has the advantages of simplicity, reliability, flexible and convenient use, low cost, stable running and high separating efficiency.
Description
Technical field
The utility model relates to a kind of chromatographic separation device, particularly a kind of three-section simulated moving bed chromatography device.
Background technology
In the sixties in 20th century, that Praxair Technology, Inc (UOP Inc.) has realized is simulation moving-bed (SimulatedMoving Bed is called for short SMB) at the industrial operation of petrochemical industry.Since the nineties in 20th century, simulated moving bed technology is introduced into pharmaceutical industry, is used for chiral drug resolution and aspects such as biological product separates, and becomes the research focus.
Simulated movable bed chromatography device is made up of the chromatographic column of some end to end one-tenth closed circuits, the regularly mobile import of flow direction by the moving phase of longshore current is simulated relative counter-current flow fixing and mobile phase with the position of outlet, and then realizes the separation of different component.This system combines chromatographic technique with simulated moving bed technology, kept advantages such as the high separation rate, low energy consumption of chromatogram, low material consumption, normal temperature operation, introduced simulated moving bed technology continuously, mechanism such as adverse current, rectifying, backflow.Introduce mechanism continuously, realize automated production, can increase substantially productive rate and efficient; Introduce countercurrent mechanism, mutually fixing and mobile being on good terms recycled, and reduces cost; Introduce rectifying, backflow mechanism, can increase separating power, improve product yield.
Generally speaking, press material liquid (Feed) and eluent (Desorbent) inlet, extract (Extract, mainly contain strong absorbed component) and raffinate (Raffinate mainly contains weak absorbed component) outlet (abbreviating E outlet and R outlet respectively as) SMBC is divided into four fundamental regions is the four-tape: be that I is with elution band between eluent inlet and the extracting liquid outlet; Be an II band extract rectifying band or a smart band between extracting liquid outlet and the material liquid inlet; Be III band absorption band between material liquid inlet and the raffinate outlet; Be IV band raffinate rectifying band or two smart bands between raffinate outlet and the eluent inlet.Arrange at least 1 above chromatographic column in each district respectively, constituted common four-tape SMBC thus, report as documents such as US 5556546, US2006/0273013A1, CN 100358606C and CN101327382.In four-tape system, add a band or an a few band, form the above simulated moving bed chromatography system of five bands, this system has the function that makes fixing regeneration mutually and separating multicomponent component, as US 6740243, US 7108789B2, CN101053705A and [J.Chromatogr.A, 2001,908,71-86] etc. document report.The IV band that saves four-tape system promptly forms the three-section simulated moving bed chromatography system, and the required chromatographic column of this system is few, the operating pressure reduction is little, and cost is low, and operation is sane.Document US 4923616 has realized independently three band SMB operational modes of I band by using rotary valve, but this valve arrangement is very complicated, it is dumb to use and cost an arm and a leg.Use the three band SMB operational modes that backflow is arranged between I band and the II band, only suitable extract is the situation of wash-out easily, document [Journal of Chromatography A, 2007,1176,69-78] and [Eng.Chem.Res.2002,41,5283-5289] adopt the solvent gradient method to finish in the case three band SMB operational modes of backflow are arranged between I band and the II band.When I band extract was difficult to wash-out, I band chromatographic column is fixing can not regenerate fully mutually, and fixedly phase carrier band extract enters the III band, be equivalent to raffinate and extract and " knock into the back ", and vicious circle, system can't be carried out steady-state operation, cause product purity to descend, separative efficiency reduces.So fixedly the circular regeneration of phase is a simulation moving-bed ten minutes important step.
The utility model content
The utility model provides a kind of three-section simulated moving bed chromatography device, significantly improves the chromatographic isolation effect.
The three-section simulated moving bed chromatography device that the utility model provides comprises: the identical chromatographic column of N root, two eluent delivery pumps, feeding liquid delivery pump, a 6N internally piloted valve, PLC or a single chip computer automatic control system, many logical, pipelines, fluid reservoir are formed, wherein 3≤N≤24.It is characterized in that this device has following structure: establish any root chromatogram column and be numbered i, 1≤i≤N is during i=1, i-1=0 refers to the N root chromatogram column, and during i=N, i+1=N+1 refers to the 1st root chromatogram column, eluent P delivery pump claims pump 1, and eluent D delivery pump claims pump 2, and feeding liquid F delivery pump claims pump 3.For the i root chromatogram column, the phase porch of flowing meets many logical I
i, the phase exit of flowing meets many logical O
iMany logical I
iThe mobile inlet mutually of i root chromatogram column is divided into four paths: article one path is by internally piloted valve P
iImport total pipeline LP with eluent P and be connected, eluent P imports total pipeline LP and is connected with fluid reservoir through pump 1, and this path is introduced eluent P; The second path is by internally piloted valve D
iImport total pipeline LD with eluent D and be connected, eluent D imports total pipeline LD and is connected with eluent D fluid reservoir CD through pump 2, and this path is introduced eluent D; Article three, path is by internally piloted valve F
iImport total pipeline LF with material liquid F and be connected, the total pipeline LF of material liquid F is connected with material liquid F fluid reservoir CF through pump 3, introduces material liquid F; Article four, path is by internally piloted valve T
I-1The many logical I of inlet mutually that flow with the i root chromatogram column
iThe many logical O of the outlet mutually of flowing with the i-1 root chromatogram column
I-1Connect, become the peripheral passage between i-1 root chromatogram column and the i root chromatogram column.The many logical I of inlet mutually that flow of the 1st root chromatogram column
1The many logical O of the outlet mutually of flowing with the N root chromatogram column
NBetween by internally piloted valve T
NBe connected to form the peripheral passage, this moment, the 1st root chromatogram column and N root chromatogram column joined end to end.Many logical O
iIt is three paths that flowing of i root chromatogram column exported mutually: article one path is by internally piloted valve R
iBe connected to raffinate R fluid reservoir CR with raffinate R delivery trunk line LR; The second path is by internally piloted valve E
iBe connected to raffinate E fluid reservoir CE with extract E delivery trunk line LE; Article three, path is by internally piloted valve T
iThe many logical O of the outlet mutually of flowing with the i root chromatogram column
iLead to I with the mobile porch mutually of i+1 root chromatogram column more
I+1Connect, become the peripheral passage between i root chromatogram column and the i+1 root chromatogram column.The many logical O of the outlet mutually of flowing of N root chromatogram column
NThe many logical I of inlet mutually that flow with the 1st root chromatogram column
1By internally piloted valve T
NConnect and also arrive the place that joins end to end.By 6 internally piloted valve P
i, D
i, F
i, E
i, R
i, T
iControl i root chromatogram column mobile inlet, exit position and circulation fluid channel status mutually, amount to 6N internally piloted valve in the whole device, by PLC or single-chip microcomputer regularly and control all internally piloted valves duty separately simultaneously, independently three to be with simulation moving-bed operational mode to be that Type B three is with simulation moving-bed to form the I band, or to have three of backflow to be with simulation moving-bed operational mode between the I-II band be that A type three is with simulation moving-bed.
Described three-section simulated moving bed chromatography device, internally piloted valve wherein is made up of magnetic valve and check (non-return) valve.
Described three-section simulated moving bed chromatography device, pipeline wherein is for isometric to the circuit of each chromatographic column input eluent P; For isometric to the circuit of each chromatographic column input eluent D; For isometric to the circuit of each chromatographic column input feeding liquid F; For isometric from the circuit of each chromatographic column output raffinate R; For isometric from the circuit of each chromatographic column output extract E; Isometric the recycle circuit between each chromatographic column.
Described three-section simulated moving bed chromatography device, pump 1 wherein, pump 2, pump 3 all are the liquid chromatography pump of carrying a kind of mobile phase, and pump 1 is connected with a fluid reservoir CP, and device is seen Fig. 1-a.
Described three-section simulated moving bed chromatography device, pump 2 wherein, pump 3 all are the liquid chromatography pump of carrying a kind of mobile phase, and pump 1 is a n unit gradient pump, is connected n=2-4 with n fluid reservoir.During n=2, device is seen Fig. 1-b.
Described three-section simulated moving bed chromatography device, chromatographic column wherein is furnished with temperature control box separately, and device is seen Fig. 1-c and 1-d.
Described three-section simulated moving bed chromatography device, be equipped with on total intake line wherein and be equipped with the detector that is equipped with flowmeter, solution concentration and purity on flowmeter, the total output pipe on filter, online degasser, the circulation line, device is seen Fig. 1-e and Fig. 1-f.
Described three-section simulated moving bed chromatography device, chromatographic column wherein are analytical column or semi-preparative column or preparative column.
Described three-section simulated moving bed chromatography device, chromatographic stationary wherein are reverse-phase chromatography filler or normal-phase chromatography filler or ion exchange resin chromatogram filler or gel exclusion chromatography filler mutually.
The three-section simulated moving bed chromatography device that the utility model provides is realized the three-section simulated moving bed chromatography operation by a cover PLC or single chip computer automatic control system, three bands comprise successively: I band-elution band, II band-rectifying band and III band-absorption band, if I band, II band and III are respectively a, b and c with required chromatographic column number, a+b+c=N, a 〉=1, b 〉=1, c 〉=1, then three tape running patterns are a-b-c, by 6 internally piloted valve P
i, D
i, F
i, E
i, R
i, T
iI root chromatogram column mobile inlet, exit position and circulation fluid channel status mutually are set, amount to 6N internally piloted valve in the whole device, by PLC or single-chip microcomputer regularly and control all internally piloted valves duty separately simultaneously, or " opening ", or " pass ", the internally piloted valve T of peripheral passage between control I band and the II band
aThe internally piloted valve D of " pass " and introducing eluent D path
A+1When " opening ", then form I band that cancellation refluxes independently three band SMB operational modes be Type B a-b-c, its operation method is: as starting point, be designated as the 1st root chromatogram column with any root chromatogram column, successively to the N root chromatogram column, the I band be set: open P by the order of connection
1, T
1-T
A-1, E
a, close the 1st all other internally piloted valves to a root chromatogram column; The II band is set: open D
A+1, T
A+1-T
A+b, close a+1 root all other internally piloted valves to the a+b root chromatogram column; The III band is set: open F
A+b+1, T
A+b+1-T
A+b+c-1, E
A+b+cClosing the a+b+1 root is all other internally piloted valves of N root chromatogram column to the a+b+c root, select switching time, make the I band, II band and III band are passed along the pillar that is directed downwards of liquid flow simultaneously, then this three band is also passed to next root pillar thereupon, this process repeats, thereby form to flow with pillar in filler mobile round about, carry out the three-section simulated moving bed chromatography operation, operational mode is Type B a-b-c, and is in service, be with at I, adopt the elution method that changes pressure, perhaps change the elution method of solvent, perhaps change the elution method of temperature, the elution method that changes solvent comprises the change solvent types, the concentration of solvent, the pH value of solution value, also comprise the solvent gradient elution method, in switching time, finish the wash-out and fixing regeneration mutually of I band extract, prepare circulation next time; The internally piloted valve T of circulation fluid T path between control I band and the II band
a" open " and introduce the internally piloted valve D of eluent D path
A+1When " pass ", then form to utilize reflux three to be with another kind of operational mode be A type a-b-c, its operation method is: as starting point, be designated as the 1st root chromatogram column with any one chromatographic column, successively to the N root chromatogram column, the I band be set: open P by the order of connection
1, T
1-T
a, E
a, close the 1st all other internally piloted valves to a root chromatogram column; The II band is set: open T
A+1-T
A+b, close a+1 root all other internally piloted valves to the a+b root chromatogram column; The III band is set: open F
A+b+1, T
A+b+1-T
A+b+c-1, E
A+b+cClosing the a+b+1 root is all other internally piloted valves of N root chromatogram column to the a+b+c root, select switching time, make the I band, II band and III band are passed along the pillar that is directed downwards of liquid flow simultaneously, then this three band is also passed to next root pillar thereupon, this process repeats, thereby form to flow with pillar in filler mobile round about, carry out the three-section simulated moving bed chromatography operation, operational mode is A type a-b-c, in service, at three bands, adopt the elution method that changes solvent, perhaps change the elution method of temperature, the elution method that changes solvent comprises the change solvent types, the concentration of solvent, the pH value of solution value also comprises the solvent gradient elution method, to shorten the cycle of operation, improve separating effect; With forming fixing eluent P wash-out, can further improve the purity of extract, and reclaim I band eluent.
The three-section simulated moving bed chromatography device that the utility model provides can move under constant temperature.
The three-section simulated moving bed chromatography device that the utility model provides is compared with existing apparatus, and its significant advantage is:
This device can realize I band independently three band SMB operational modes be Type B three tape running mechanism, or three band SMB operational modes of backflow are arranged between I band and the II band is A type three tape running mechanism, can select different mode according to the complexity of extract wash-out.When extract is difficult to wash-out, use Type B three band SMB, adopt the elution method that changes pressure, perhaps change the elution method of solvent, perhaps change the elution method of temperature, in switching time, can realize wash-out, the fixedly regeneration of phase of the extract of I band elution band, therefore and the stable operation of safeguard work system, and the assurance product purity; During the more difficult wash-out of extract, use A type three band SMB, adopt the elution method that changes solvent, perhaps change the elution method of temperature, can shorten the cycle of operation, improve separating effect; When extract is easy to wash-out, use A type three band SMB to adopt the fixing eluent P elution method of forming, can further improve the purity of extract, and reclaim I band eluent.Device of the present invention is simple and reliable, use is flexible, easy to operate, cost is low, stable, for resolving chiral medicine, separating bio product and chemical products provide efficient separation equipment and means.
Description of drawings
Fig. 1-a is the three-section simulated moving bed chromatography device figure of the N root chromatogram column that is connected with a fluid reservoir CP of pump 1.
LP-eluent P imports total pipeline, and LD-eluent D imports total pipeline, and LF-material liquid F imports total pipeline, LE-extract E delivery trunk line, LR-raffinate R delivery trunk line, the delivery pump of pump 1-eluent P, the delivery pump of pump 2-eluent D, the delivery pump of pump 3-material liquid F, the fluid reservoir of CP-eluent P, the fluid reservoir of CD-eluent D, the fluid reservoir of CF-material liquid F, the fluid reservoir of CE-extract E, the fluid reservoir of CR-raffinate R, i-i root chromatogram column, P
iThe eluent P inlet internally piloted valve of-Di i root chromatogram column, D
iThe eluent D inlet internally piloted valve of-Di i root chromatogram column, F
iThe material liquid F inlet internally piloted valve of-Di i root chromatogram column, T
iThe mobile phase exit of-control connection i root chromatogram column and the circulation internally piloted valve of the mobile porch mutually route profiling of (i+1) root chromatogram column, R
iThe raffinate outlet internally piloted valve of-Di i root chromatogram column, E
iThe extracting liquid outlet internally piloted valve of-Di i root chromatogram column, I
iThe five-way of-Di i root chromatogram column, O
iThe four-way of-Di i root chromatogram column.
Fig. 1-b is the three-section simulated moving bed chromatography device figure of pump 1 for the N root chromatogram column of gradient pump.
Pump 1-binary gradient pump, CP
AThe fluid reservoir of-solution A, CP
B-solution B fluid reservoir.
Fig. 1-c be pump 1 be connected with a fluid reservoir CP be furnished with the three-section simulated moving bed chromatography device figure of the N root chromatogram column of temperature control box separately.
H
iThe temperature control box of-Di i root chromatogram column.
Fig. 1-d is the three-section simulated moving bed chromatography device figure of pump 1 for the N root chromatogram column of being furnished with temperature control box separately of gradient pump.
Fig. 1-e is that pump 1 is connected with a fluid reservoir CP, is equipped with on total intake line and is equipped with the three-section simulated moving bed chromatography device figure that is equipped with the N root chromatogram column of flowmeter, solution concentration and purity detector on flowmeter, the total output pipe on filter, online degasser, the circulation line.
DG1, DG2, DG3 are respectively online degasser, F1, F2, F3 are respectively the filter of eluent P, eluent D, material liquid F, M1, M2, M3 are respectively the flowmeter of circulation line, extract E delivery trunk line, raffinate R delivery trunk line, and M4 and M5 are respectively the detector of extract E and raffinate R solution concentration and purity.
Fig. 1-f is that pump 1 is equipped with the three-section simulated moving bed chromatography device figure that is equipped with the N root chromatogram column that is equipped with flowmeter, solution concentration and purity detector on flowmeter, the output pipe on filter, online degasser, the circulation line on total intake line of gradient pump.
The online degasser of the binary channels of DG1AB-solution A and solution B.
Fig. 2-a is the three-section simulated moving bed chromatography device figure of 8 root chromatogram columns that are connected with a fluid reservoir CP of pump 1.
Fig. 2-b is the three-section simulated moving bed chromatography device figure of pump 1 for 8 root chromatogram columns of binary gradient pump.
Fig. 2-c be pump 1 be connected with a fluid reservoir CP be furnished with the three-section simulated moving bed chromatography device figure of 8 root chromatogram columns of temperature control box separately.
Fig. 2-d is the three-section simulated moving bed chromatography device figure of pump 1 for 8 root chromatogram columns of being furnished with temperature control box separately of gradient pump.
Be equipped with on total intake line that Fig. 2-e is a pump 1 with a fluid reservoir CP is connected and be equipped with the three-section simulated moving bed chromatography device figure that is equipped with 8 root chromatogram columns of flowmeter, solution concentration and purity detector on flowmeter, the total output pipe on filter, online degasser, the circulation line.
Fig. 2-f is that pump 1 is equipped with the three-section simulated moving bed chromatography device figure that is equipped with the N root chromatogram column of flowmeter, solution concentration and purity detector on flowmeter, the total output pipe for being equipped with on total intake line of gradient pump on filter, online degasser, the circulation line.
Fig. 3-a is the operation schematic diagram (add heavy line and be the operation original state) of 8 root chromatogram column three-section simulated moving bed chromatography 2-3-3 (B).
Fig. 3-b is the operation schematic diagram (add heavy line and be the operation original state) of 8 root chromatogram column three-section simulated moving bed chromatography 2-2-4 (A).
The specific embodiment
Three-section simulated moving bed chromatography device embodiment 1
Shown in Fig. 2-a, pump 1 comprises with the three-section simulated moving bed chromatography device of 8 root chromatogram columns that fluid reservoir CP connects: 8 identical chromatographic columns, two eluent delivery pumps, feeding liquid delivery pump, 6 * 8 internally piloted valves, PLC automatic control system, many logical, pipelines, 3 fluid reservoirs; This device has its following structure, establishes any root chromatogram column and is numbered i, and 1≤i≤8 are during i=1, i-1=0 refers to the 8th root chromatogram column, and during i=8, i+1=8+1 refers to the 1st root chromatogram column, eluent P delivery pump claims pump 1, and eluent D delivery pump claims pump 2, and feeding liquid F delivery pump claims pump 3; For the i root chromatogram column, the phase porch of flowing meets many logical I
i, the phase exit of flowing meets many logical O
iMany logical I
iThe mobile inlet mutually of i root chromatogram column is divided into four paths: article one path is by internally piloted valve P
iImport total pipeline LP with eluent P and be connected, eluent P imports total pipeline LP and is connected with eluent P fluid reservoir CP through pump 1, and this path is introduced eluent P, and the second path is by internally piloted valve D
iImport total pipeline LD with eluent D and be connected, eluent D imports total pipeline LD and is connected with eluent D fluid reservoir CD through pump 2, and this path is introduced eluent D, and the 3rd path is by internally piloted valve F
iImport total pipeline LF with material liquid F and be connected, the total pipeline LF of material liquid F is connected with material liquid F fluid reservoir CF through pump 3, introduces material liquid F, and the 4th path is by internally piloted valve T
I-1The many logical I of inlet mutually that flow with the i root chromatogram column
iThe many logical O of the outlet mutually of flowing with the i-1 root chromatogram column
I-1Connect, become the peripheral passage between i-1 root chromatogram column and the i root chromatogram column, the many logical I of inlet mutually that flow of the 1st root chromatogram column
1The many logical O of the outlet mutually of flowing with the 8th root chromatogram column
8Between by internally piloted valve T
8Be connected to form the peripheral passage, this moment, the 1st root chromatogram column and the 8th root chromatogram column joined end to end; Many logical O
iIt is three paths that flowing of i root chromatogram column exported mutually: article one path is by internally piloted valve R
iBe connected to raffinate R fluid reservoir CR with raffinate R delivery trunk line LR, the second path is by internally piloted valve E
iBe connected to raffinate E fluid reservoir CE with raffinate E delivery trunk line LE, the 3rd path is by internally piloted valve T
iThe many logical O0 of the outlet mutually of flowing with the i root chromatogram column
iLead to I with the mobile porch mutually of i+1 root chromatogram column more
I+1Connect, become the peripheral passage between i root chromatogram column and the i+1 root chromatogram column, the many logical O of the outlet mutually of flowing of the 8th root chromatogram column
8The many logical I of inlet mutually that flow with the 1st root chromatogram column
1By internally piloted valve T
8Connect the same place that joins end to end that arrives; By 6 internally piloted valve P
i, D
i, F
i, E
i, R
i, T
iI root chromatogram column mobile inlet, exit position and circulation fluid channel status mutually are set, amount to 6 * 8 internally piloted valves in the whole device, by PLC or single-chip microcomputer regularly and control all internally piloted valves duty separately simultaneously, independently three to be with simulation moving-bed operational mode to be that Type B three is with simulation moving-bed to form the I band, or to have three of backflow to be with simulation moving-bed operational mode between the I-II band be that A type three is with simulation moving-bed.
Three-section simulated moving bed chromatography device embodiment 2
Shown in Fig. 2-b, three of 8 root chromatogram columns that a kind of pump 1 is a gradient pump are with simulation moving-bed device, and pump 1 is two yuan of gradient pumps, with the fluid reservoir CP of solution A
AFluid reservoir CP with solution B
BConnect, other structure is with embodiment 1.
Three-section simulated moving bed chromatography device embodiment 3
Shown in Fig. 2-c, a kind of pump 1 is connected with a fluid reservoir CP is furnished with the three-section simulated moving bed chromatography device of 8 root chromatogram columns of temperature control box separately, and 8 root chromatogram columns are furnished with temperature control box H separately
1-H
8, other structure is with embodiment 1.
Three-section simulated moving bed chromatography device embodiment 4
Shown in Fig. 2-d, a kind of pump 1 is the three-section simulated moving bed chromatography device figure of 8 root chromatogram columns of temperature control box separately that is furnished with of gradient pump, and 8 root chromatogram columns are furnished with temperature control box H separately
1-H
8, other structure is with embodiment 2.
Three-section simulated moving bed chromatography device embodiment 5
Shown in Fig. 2-e, be equipped with on a kind of pump 1 and the total intake line that a fluid reservoir CP is connected and be equipped with three of 8 root chromatogram columns that are equipped with flowmeter, solution concentration and purity detector on flowmeter, the total output pipe on filter, online degasser, the circulation line and be with simulation moving-bed installation drawing.Fluid reservoir CP is connected with pump 1 through online degasser DG1, and pump 1 is imported total pipeline LP through filter F1 with eluent P and is connected; Fluid reservoir CD is connected with pump 2 through online degasser DG2, and pump 2 is imported total pipeline LD through filter F2 with eluent D and is connected; Fluid reservoir CF is connected with pump 3 through online degasser DG3, and pump 3 is imported total pipeline LF through filter F3 with material liquid F and is connected, and the also available three-channel online degasser of above-mentioned three online degassers replaces; As on the 8th circulation line flowmeter M1 is being set on the circulation line arbitrarily; Extract E delivery trunk line LE links to each other with the fluid reservoir CE of extract E through flowmeter M2, solution concentration and purity detector M4, raffinate R delivery trunk line LR links to each other with the fluid reservoir CR of raffinate R through flowmeter M3, solution concentration and purity detector M5, and other structure is with embodiment 1.
Three-section simulated moving bed chromatography device embodiment 6
Shown in Fig. 2-f, a kind of pump 1 is equipped with the three-section simulated moving bed chromatography device that is equipped with 8 root chromatogram columns of flowmeter, solution concentration and purity detector on flowmeter, the total output pipe for being equipped with on total intake line of gradient pump on filter, online degasser, the circulation line.Pump 1 is two yuan of gradient pumps, the fluid reservoir CP of solution A
AFluid reservoir CP with solution B
BBe connected with pump 1 through an online degasser DG1AB of binary channels respectively, pump 1 is imported total pipeline LP through filter F1 with eluent P and is connected, and other structure is with embodiment 5.
Patent of the present invention is fit to the situation of 3≤N≤24, and the capacity of chromatographic column sum N and pump, the pressure of post fall, the purity requirement of the separating power of single-column and separated object is relevant.
Chromatographic column is analytical column or semi-preparative column or preparative column and the corresponding supporting use of liquid chromatography pump in above-mentioned all devices.
The fixing of chromatographic column is normal-phase chromatography filler or reverse-phase chromatography filler or ion exchange resin chromatogram filler or gel exclusion chromatography filler mutually in above-mentioned all devices.
In above-mentioned all devices, the PLC automatic control system can replace with single chip computer automatic control system.
Three band SMB systems with 8 root chromatogram columns are that example illustrates its operational mode and setting.It has plurality of operating modes, comprising: 1-1-6; 1-6-1; 6-1-1; 1-2-5; 1-5-2; 2-1-5; 5-1-2; 2-5-1; 5-2-1; 1-3-4; 1-4-3; 3-1-4; 4-1-3; 4-3-1; 3-4-1; 2-2-4; 2-4-2; 4-2-2; 2-3-3; 3-2-3; 3-3-2.
Shown in Fig. 3-a, with Type B 2-3-3 mode declaration pattern specification I band three band SMB operational modes independently: with any one chromatographic column as starting point, be designated as the 1st root chromatogram column by the order of connection successively to the 8th root chromatogram column.The I band is set: open P
1, T
1, E
2, close the 1st, all other internally piloted valves of the 2nd root chromatogram column, I band chromatographic column number is 2; The II band is set: open D
3, T
3, T
4, T
5, close the 3rd all other internally piloted valves to the 5th root chromatogram column, II band chromatographic column number is 3; The III band is set: open F
6, T
6, T
7, R
8, close the 6th all other internally piloted valves to the 8th root chromatogram column, III band chromatographic column number is 3.Select suitable switching time, I band, II band and III band are passed to next root pillar along the direction (being the order that chromatographic column is connected successively) of liquid flow simultaneously, then this three band is also passed to next root pillar thereupon, thereby form to flow with pillar in filler mobile round about, carry out the three-section simulated moving bed chromatography operation, operational mode is designated as 2-3-3 (B).
Shown in Fig. 3-b, the three band SMB operational modes that reflux with A type 2-2-4 mode declaration pattern specification utilization: with any one chromatographic column as starting point, be designated as the 1st root chromatogram column by the order of connection successively to the 8th root chromatogram column.The I band is set: open P
1, T
1, T
2, E
2, close the 1st, all other internally piloted valves of the 2nd root chromatogram column; The II band is set: open T
3, T
4, close the 3rd, all other internally piloted valves of the 4th root chromatogram column; The III band is set: open F
5, T
5-T
7, E
8, close the 5th all other internally piloted valves to the 8th root chromatogram column.Select suitable switching time, I band, II band and III band are passed to next root pillar along the direction (being the order that chromatographic column is connected successively) of liquid flow simultaneously, then this three band is also passed to next root pillar thereupon, thereby form to flow with pillar in filler mobile round about, carry out the three-section simulated moving bed chromatography operation, operational mode is designated as 2-2-4 (A).
Therefore, three operational modes with simulation moving-bed Type B a-b-c of 8 root chromatogram columns composition are: 1-1-6 (B); 1-6-1 (B); 6-1-1 (B); 1-2-5 (B); 1-5-2 (B); 2-1-5 (B); 5-1-2 (B); 2-5-1 (B); 5-2-1 (B); 1-3-4 (B); 1-4-3 (B); 3-1-4 (B); 4-1-3 (B); 4-3-1 (B); 3-4-1 (B); 2-2-4 (B); 2-4-2 (B); 4-2-2 (B); 2-3-3 (B); 3-2-3 (B); 3-3-2 (B).Three operational modes with simulation moving-bed A type a-b-c that 8 root chromatogram columns are formed are: 1-1-6 (A); 1-6-1 (A); 6-1-1 (A); 1-2-5 (A); 1-5-2 (A); 2-1-5 (A); 5-1-2 (A); 2-5-1 (A); 5-2-1 (A); 1-3-4 (A); 1-4-3 (A); 3-1-4 (A); 4-1-3 (A); 4-3-1 (A); 3-4-1 (A); 2-2-4 (A); 2-4-2 (A); 4-2-2 (A); 2-3-3 (A); 3-2-3 (A); 3-3-2 (A).
Claims (9)
1. three-section simulated moving bed chromatography device, comprise the identical chromatographic column of N root, two eluent delivery pumps, a feeding liquid delivery pump, 6N internally piloted valve, PLC or single chip computer automatic control system, how logical, pipeline, fluid reservoir, 3≤N≤24 wherein, it is characterized in that this device has following structure: establish any root chromatogram column and be numbered i, 1≤i≤N, during i=1, i-1=0 refers to the N root chromatogram column, during i=N, i+1=N+1 refers to the 1st root chromatogram column, and eluent P delivery pump claims pump 1, eluent D delivery pump claims pump 2, feeding liquid F delivery pump claims pump 3, and for the i root chromatogram column, the phase porch of flowing meets many logical I
i, the phase exit of flowing meets many logical O
i, lead to I more
iThe mobile inlet mutually of i root chromatogram column is divided into four paths: article one path is by internally piloted valve P
iImport total pipeline LP with eluent P and be connected, eluent P imports total pipeline LP and is connected with fluid reservoir through pump 1, and this path is introduced eluent P; The second path is by internally piloted valve D
iImport total pipeline LD with eluent D and be connected, eluent D imports total pipeline LD and is connected with eluent D fluid reservoir CD through pump 2, and this path is introduced eluent D; Article three, path is by internally piloted valve F
iImport total pipeline LF with material liquid F and be connected, the total pipeline LF of material liquid F is connected with material liquid F fluid reservoir CF through pump 3, introduces material liquid F; Article four, path is by internally piloted valve T
I-1The many logical I of inlet mutually that flow with the i root chromatogram column
iThe many logical O of the outlet mutually of flowing with the i-1 root chromatogram column
I-1Connect, become the peripheral passage between i-1 root chromatogram column and the i root chromatogram column, the many logical I of inlet mutually that flow of the 1st root chromatogram column
1The many logical O of the outlet mutually of flowing with the N root chromatogram column
NBetween by internally piloted valve T
NBe connected to form the peripheral passage, this moment, the 1st root chromatogram column and N root chromatogram column joined end to end, and led to O more
iIt is three paths that flowing of i root chromatogram column exported mutually: article one path is by internally piloted valve R
iBe connected to raffinate R fluid reservoir CR with raffinate R delivery trunk line LR; The second path is by internally piloted valve E
iBe connected to raffinate E fluid reservoir CE with extract E delivery trunk line LE; Article three, path is by internally piloted valve T
iThe many logical O of the outlet mutually of flowing with the i root chromatogram column
iLead to I with the mobile porch mutually of i+1 root chromatogram column more
I+1Connect, become the peripheral passage between i root chromatogram column and the i+1 root chromatogram column, the many logical O of the outlet mutually of flowing of N root chromatogram column
NThe many logical I of inlet mutually that flow with the 1st root chromatogram column
1By internally piloted valve T
NConnection also arrives the place that joins end to end, by 6 internally piloted valve P
i, D
i, F
i, E
i, R
i, T
iControl i root chromatogram column mobile inlet, exit position and circulation fluid channel status mutually, amount to 6N internally piloted valve in the whole device, by PLC or single-chip microcomputer regularly and control all internally piloted valves duty separately simultaneously, independently three to be with simulation moving-bed operational mode to be that Type B three is with simulation moving-bed to form the I band, or to have three of backflow to be with simulation moving-bed operational mode between the I-II band be that A type three is with simulation moving-bed.
2. three-section simulated moving bed chromatography device according to claim 1 is characterized in that: said internally piloted valve is made up of magnetic valve and check (non-return) valve.
3. three-section simulated moving bed chromatography device according to claim 1 is characterized in that: said pipeline, and isometric to the circuit of each chromatographic column input eluent P; Circuit to each chromatographic column input eluent D is isometric; Circuit to each chromatographic column input feeding liquid F is isometric; Isometric from the circuit of each chromatographic column output raffinate R; Isometric from the circuit of each chromatographic column output extract E; Recycle circuit between each chromatographic column is isometric.
4. three-section simulated moving bed chromatography device according to claim 1 is characterized in that: said pump 1, pump 2, pump 3 all are the liquid chromatography pump of carrying a kind of mobile phase, and pump 1 is connected with a fluid reservoir CP.
5. three-section simulated moving bed chromatography device according to claim 1 is characterized in that: said pump 2, pump 3 all are the liquid chromatography pump of carrying a kind of mobile phase.
6. three-section simulated moving bed chromatography device according to claim 1 is characterized in that: said chromatographic column is furnished with temperature control box separately.
7. three-section simulated moving bed chromatography device according to claim 1, it is characterized in that: be equipped with filter, online degasser on said total intake line, be equipped with flowmeter on the circulation line, be equipped with the detector of flowmeter, solution concentration and purity on total output pipe.
8. three-section simulated moving bed chromatography device according to claim 1 is characterized in that: said chromatographic column is analytical column or semi-preparative column or preparative column.
9. three-section simulated moving bed chromatography device according to claim 1 is characterized in that: the fixing of said chromatographic column is reverse-phase chromatography filler or normal-phase chromatography filler or ion exchange resin chromatogram filler or gel exclusion chromatography filler mutually.
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| Application Number | Priority Date | Filing Date | Title |
|---|---|---|---|
| CN 200920277023 CN201618442U (en) | 2009-12-08 | 2009-12-08 | Three-band analogue moving bed chromatogram device |
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| Application Number | Priority Date | Filing Date | Title |
|---|---|---|---|
| CN 200920277023 CN201618442U (en) | 2009-12-08 | 2009-12-08 | Three-band analogue moving bed chromatogram device |
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| CN201618442U true CN201618442U (en) | 2010-11-03 |
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| CN 200920277023 Expired - Lifetime CN201618442U (en) | 2009-12-08 | 2009-12-08 | Three-band analogue moving bed chromatogram device |
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Cited By (5)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| CN106237654A (en) * | 2016-09-19 | 2016-12-21 | 辽宁科技大学 | A kind of method of the online deep regenerative of simulated moving bed chromatography post |
| CN109432823A (en) * | 2018-11-14 | 2019-03-08 | 内蒙古伊泰煤基新材料研究院有限公司 | It is a kind of suitable for the temperature control system of Simulation moving bed and the temprature control method of Simulation moving bed |
| CN109432822A (en) * | 2018-11-14 | 2019-03-08 | 内蒙古伊泰煤基新材料研究院有限公司 | A kind of mobile bed apparatus of efficient simulation and efficient simulation moving bed process |
| CN108840793B (en) * | 2018-05-28 | 2021-06-15 | 辽宁科技大学 | Method for preparing gamma-thujaplicin by using simulated moving bed chromatography |
| CN115485046A (en) * | 2020-05-14 | 2022-12-16 | 奥加诺株式会社 | Simulated moving bed mode chromatographic separation method and simulated moving bed mode chromatographic separation system |
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2009
- 2009-12-08 CN CN 200920277023 patent/CN201618442U/en not_active Expired - Lifetime
Cited By (10)
| Publication number | Priority date | Publication date | Assignee | Title |
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| CN106237654A (en) * | 2016-09-19 | 2016-12-21 | 辽宁科技大学 | A kind of method of the online deep regenerative of simulated moving bed chromatography post |
| CN106237654B (en) * | 2016-09-19 | 2018-04-17 | 辽宁科技大学 | A kind of method of the online deep regenerative of Simulated Moving Bed Chromatography column |
| CN108840793B (en) * | 2018-05-28 | 2021-06-15 | 辽宁科技大学 | Method for preparing gamma-thujaplicin by using simulated moving bed chromatography |
| CN109432823A (en) * | 2018-11-14 | 2019-03-08 | 内蒙古伊泰煤基新材料研究院有限公司 | It is a kind of suitable for the temperature control system of Simulation moving bed and the temprature control method of Simulation moving bed |
| CN109432822A (en) * | 2018-11-14 | 2019-03-08 | 内蒙古伊泰煤基新材料研究院有限公司 | A kind of mobile bed apparatus of efficient simulation and efficient simulation moving bed process |
| CN109432822B (en) * | 2018-11-14 | 2023-09-29 | 内蒙古伊泰煤基新材料研究院有限公司 | Efficient simulated moving bed equipment and efficient simulated moving bed process |
| CN109432823B (en) * | 2018-11-14 | 2023-11-21 | 内蒙古伊泰煤基新材料研究院有限公司 | Temperature control system suitable for simulated moving bed and temperature control method of simulated moving bed |
| US11980833B2 (en) | 2018-11-14 | 2024-05-14 | Inner Mongolia Yitai Coal-Based New Materials Research Institute Co., Ltd. | Efficient simulated moving bed device and efficient simulated moving bed process |
| CN115485046A (en) * | 2020-05-14 | 2022-12-16 | 奥加诺株式会社 | Simulated moving bed mode chromatographic separation method and simulated moving bed mode chromatographic separation system |
| CN115485046B (en) * | 2020-05-14 | 2024-03-12 | 奥加诺株式会社 | Simulated moving bed type chromatographic separation method and simulated moving bed type chromatographic separation system |
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