IPC분류정보
국가/구분 |
United States(US) Patent
등록
|
국제특허분류(IPC7판) |
|
출원번호 |
US-0273801
(2011-10-14)
|
등록번호 |
US-8441629
(2013-05-14)
|
우선권정보 |
EP-09157910 (2009-04-15) |
발명자
/ 주소 |
- Kolesnychenko, Aleksey
- De Vries, Jorrit E.
- Versleegers, Jozef C. M.
- De Jong, Michiel
- Haddeman, Theodoor B. J.
- Stroucken, Louis
|
출원인 / 주소 |
|
대리인 / 주소 |
|
인용정보 |
피인용 횟수 :
4 인용 특허 :
72 |
초록
▼
An optical detection system for monitoring real-time PCR reactions in a plurality of sample chambers with a plurality of optical units is provided. Due to a relative movement, the optical units are relative to the sample chambers, color multiplexing and space multiplexing are combined for optically
An optical detection system for monitoring real-time PCR reactions in a plurality of sample chambers with a plurality of optical units is provided. Due to a relative movement, the optical units are relative to the sample chambers, color multiplexing and space multiplexing are combined for optically detecting pathogens in a sample during the process of the PCR and delivering a quantitative result.
대표청구항
▼
1. An optical multiplexing system for detecting sample components in at least two different sample chambers, the system comprising: a first optical unit for detecting a product of a first polymerase chain reaction (PCR), wherein the first optical unit comprises a first light source and a first detec
1. An optical multiplexing system for detecting sample components in at least two different sample chambers, the system comprising: a first optical unit for detecting a product of a first polymerase chain reaction (PCR), wherein the first optical unit comprises a first light source and a first detector;a second optical unit for detecting a product of a second polymerase chain reaction (PCR), wherein the second optical unit comprises a second light source and a second detector, wherein the first optical unit and the second optical unit are spatially separated from each other, wherein the system receives at least two sample chambers to be received at positions corresponding to the first and second optical units so that (a) the first and second light sources, respectively, simultaneously illuminate the at least two sample chambers and (b) the first and second detectors, respectively, simultaneously receive light from the at least two sample chambers, said first and second optical units simultaneously performing first and second optical measurement using two different optical wavelengths at said two spatially separated sample chambers, andwherein the system is adapted for a relative movement of the first optical unit and the second optical unit relative to the at least two sample chambers;a first heater associated with a first sample chamber of the at least two sample chambers, said first heater creating a first temperature progression at the first sample chamber;a second heater associated with a second sample chamber of the at least two sample chambers, said second heater creating a second temperature progression at the second sample chamber; anda control unit for receiving a PCR protocol, wherein said control unit controls the first and second heaters according to the PCR protocol to cause real time PCR reactions in the first and second sample chambers, said control unit simultaneously quantifying a targeted and amplified DNA molecule by relative movement of the first optical unit and second optical unit relative to the at least two sample chambers. 2. The optical multiplexing system according to claim 1, further comprising a motor, wherein the motor is adapted to cause the relative movement. 3. The optical multiplexing system according to claim 2, further comprising a rotation frame, wherein the first and second optical units are fixed at the rotation frame and wherein the motor causes the relative movement by rotating the rotation frame. 4. The optical multiplexing system according to claim 1, wherein the relative movement is a rotating movement. 5. The optical multiplexing system according to claim 1, wherein the relative movement is a linear movement. 6. The optical multiplexing system according to claim 1, wherein said first and second heaters cause a thermal cycling in the first and second sample chambers. 7. A molecular diagnostic device for analyzing a sample, the device comprising an optical multiplexing system according to claim 1. 8. The optical multiplexing system according to claim 1, wherein the first and second heaters have an optical transparency greater than 80% in a spectral range between 300 nm and 800 nm wavelength. 9. The optical multiplexing system according to claim 1, wherein the first and second heaters have a negligible autofluoresence at excitation wavelengths between 300 nm and 800 nm. 10. A method for detecting sample components in at least two different sample chambers, the method comprising the steps of: receiving at least two sample chambers, each sample chamber having a sample;aligning a first sample chamber of the at least two sample chambers with a first optical unit comprised of a first light source and a first detector;aligning a second sample chamber of the at least two sample chambers with a second optical unit comprised of a second light source and a second detector, wherein the first optical unit and the second optical unit are spatially separated from each other;simultaneously performing (i) a first optical measurement of a first sample chamber of the at least two sample chambers using a first optical wavelength and (ii) a second optical measurement of a second sample chamber of the at least two sample chambers using a second optical wavelength, wherein simultaneously performing the first and second optical measurements includes: (a) simultaneously illuminating the at least two sample chambers using the first and second light sources, respectively, and(b) simultaneously receiving light from the at least two sample chambers using the first and second detectors, respectively;moving the first optical unit and the second optical unit relative to the at least two sample chambers so as to cause an alignment of the first sample chamber with the second optical unit and an alignment of the second sample chamber with the first optical unit;heating the first sample chamber of the at least two sample chambers with a first heater to create a first temperature progression at the first sample chamber;heating the second sample chamber of the at least two sample chambers with a second heater to create a second temperature progression at the second sample chamber; andcontrolling the first and second heaters according to a PCR protocol to cause real time PCR reactions in the first and second sample chambers, and simultaneously quantifying a targeted and amplified DNA molecule by relative movement of the first optical unit and the second optical unit relative to the at least two sample chambers. 11. The method according to claim 10, further comprising the steps of: performing a third optical measurement of the first sample chamber with the second optical unit; andperforming a fourth optical measurement of the second sample chamber with the first optical unit. 12. The method according to claim 10, further comprising: causing thermal cycling in the first and second sample chambers with the first and second heaters. 13. A computer program element characterized by being adapted, when in use on a general purpose computer, to cause the computer to perform the steps of: aligning a first sample chamber with a first optical unit comprising a first light source and a first detector;aligning a second sample chamber with a second optical unit comprising a second light source and a second detector, wherein the first optical unit and the second optical unit are spatially separated from each other and the first optical unit and second optical unit are physically linked parts of an optical detection system;simultaneously performing (i) a first optical measurement of the first sample chamber using a first optical wavelength and (ii) a second optical measurement of a second sample chamber using a second optical wavelength, wherein simultaneously performing the first and second optical measurements includes: (a) simultaneously illuminating the first and second sample chambers using the first and second light sources, respectively, and(b) simultaneously receiving light from the first and second sample chambers using the first and second detectors, respectively;heating the first sample chamber with a first heater to create a first temperature progression at the first sample chamber;heating the second sample chamber with a second heater to create a second temperature progression at the second sample chamber;controlling the first and second heaters according to a PCR protocol to cause real time PCR reactions in the first and second sample chambers, and simultaneously quantifying a targeted and amplified DNA molecule by relative movement of the first optical unit and the second optical unit relative to the first and second sample chambers; andmoving the first optical unit and the second optical unit relative to the first and second sample chambers so as to cause an alignment of the first sample chamber with the second optical unit and an alignment of the second sample chamber with the first optical unit. 14. A non-transitory computer readable medium storing instructions of a computer program which, when executed by a computer, result in the performance of the steps according to claim 13. 15. An optical multiplexing system for detecting sample components in at least two sample chambers, the system comprising: a first optical unit having a first light source and a first detector, said first optical unit detecting a product of a first polymerase chain reaction (PCR);a second optical unit having a second light source and a second detector, said second optical unit detecting a product of a second polymerase chain reaction (PCR), wherein the second optical unit is spatially separated from the first optical unit;a first heater associated with a first sample chamber of the at least two sample chambers, said first heater creating a first temperature progression at the first sample chamber;a second heater associated with a second sample chamber of the at least two sample chambers, said second heater creating a second temperature progression at the second sample chamber;a rotation frame having the first and second optical units fixed thereto;a motor adapted to rotate the rotation frame so as to cause the first and second optical units to move between a first position and a second position,wherein, when in the first position, the first optical unit is positioned with respect to a first sample chamber and the first heater so that the first light source illuminates and the first detector receives light from the first sample chamber, while the second optical unit is positioned with respect to a second sample chamber and the second heater so that the second light source illuminates and the second detector receives light from the second sample chamber, andsaid first and second optical units simultaneously illuminate the at least two sample chambers, and the first and second detectors simultaneously receive light from the at least two sample chambers, wherein said first and second optical units simultaneously perform first and second optical measurement using two different optical wavelengths at said at least two sample chambers; anda control unit for receiving a PCR protocol, wherein said control unit controls the first and second heaters according to the PCR protocol to cause real time PCR reactions in the first and second sample chambers, said control unit simultaneously quantifying a targeted and amplified DNA molecule by relative movement of the first optical unit and second optical unit relative to the at least two sample chambers. 16. The optical multiplexing system according to claim 15, wherein, when in the second position, the first optical unit is positioned with respect to the second sample chamber and the second heater so that the first light source illuminates and the first detector receives light from the second sample chamber, while the second optical unit is positioned with respect to the first sample chamber and the first heater so that the second light source illuminates and the second detector receives light from the first sample chamber. 17. The optical multiplexing system according to claim 15, wherein the first and second heaters are optically transparent to said first and second light sources, said first and second heaters have an optical transparency greater than 80% in a spectral range between 300 nm and 800 nm wavelength. 18. The optical multiplexing system according to claim 15, wherein the first and second heaters have a negligible autofluoresence at excitation wavelengths between 300 nm and 800 nm. 19. An optical multiplexing system for detecting sample components in at least two sample chambers, the system comprising: a first optical unit comprising a first light source and a first detector, said first optical unit detecting a product of a first polymerase chain reaction (PCR);a second optical unit comprising a second light source and a second detector, said second optical unit detecting a product of a second polymerase chain reaction (PCR), wherein the first and second optical units are spatially separated from each other, wherein the system receives at least two sample chambers to be received at positions corresponding to the first and second optical units so that the first and second light sources, respectively, simultaneously illuminate the at least two sample chambers, and the first and second detectors, respectively, simultaneously receive light from the at least two sample chambers, said first and second optical units simultaneously performing first and second optical measurements using two different optical wavelengths at said two spatially separated sample chambers;a first heater associated with a first sample chamber of the at least two sample chambers, said first heater creating a first temperature progression at the first sample chamber;a second heater associated with a second sample chamber of the at least two sample chambers, said second heater creating a second temperature progression at the second sample chamber; anda control unit for receiving a PCR protocol, wherein said control unit controls the first and second heaters according to the PCR protocol to cause real time PCR reactions in the first and second sample chambers, said control unit simultaneously quantifying a targeted and amplified DNA molecule by relative movement of the first optical unit and second optical unit relative to the at least two sample chambers,wherein the system is adapted for: performing a first optical measurement of the first sample chamber with the first optical unit,performing a second optical measurement of the second sample chamber with the second optical unit, anda relative movement of the first and second optical units relative to the at least two sample chambers in order to get to a second stationary position in which the first optical unit is aligned with the second sample chamber and the second optical unit is aligned with the first sample chamber.
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