CN106074574A - A kind of medicine for treating the cancer of the esophagus and using method - Google Patents

A kind of medicine for treating the cancer of the esophagus and using method Download PDF

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CN106074574A
CN106074574A CN201510205305.0A CN201510205305A CN106074574A CN 106074574 A CN106074574 A CN 106074574A CN 201510205305 A CN201510205305 A CN 201510205305A CN 106074574 A CN106074574 A CN 106074574A
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Abstract

A kind of medicine for treating the cancer of the esophagus of the present invention contains 4-[4-[(4'-chlorine [1,1'-biphenyl]-2-base) methyl]-1-piperazinyl]-N-[[4-[[(1R)-3-(dimethylamino)-1-[(thiophenyl) methyl] propyl group] amino]-3-nitrobenzophenone] sulfonyl] benzamide (chemical formula C42H45ClN6O5S2, code name ABT-737) or the compound with described ABT-737 as basic system, it is used for treating the cancer of the esophagus, or as Chemotherapy in Esophageal Cancer and radiocurable hypersitization medicine.A kind of medicine for treating the cancer of the esophagus of the present invention, by the mechanism of induced tumor apoptosis, reduces Chemotherapy in Esophageal Cancer and (or) radiotherapy tolerance, improves the result for the treatment of of the cancer of the esophagus, is conducive to improving patient with esophageal carcinoma cure rate and total existence.

Description

A kind of medicine for treating the cancer of the esophagus and using method
Technical field
The present invention relates to a kind of medicine treating tumour, specifically one is used for treating the cancer of the esophagus, or as Chemotherapy in Esophageal Cancer and radiocurable hypersitization medicine;Particularly the tolerance of the chemotherapy of the esophageal squamous cell carcinoma of 5, radiotherapy or chemicotherapy is more than to sodium hydrogen interchange channel 9 albumen (being called for short NHE9) immunohistochemical staining index, strengthens the result for the treatment of of chemotherapy, radiotherapy or chemicotherapy.
Background technology
The cancer of the esophagus is one of common cancer in the world, and annual whole world new cases 45.6 ten thousand case, death is more than 400,000 cases.Annual new cases 25.9 ten thousand case of China, dead 21.1 ten thousand cases, wherein 95% is squama cancer.At present, surgical intervention is the essential therapeutic arsenals of China's cancer of the esophagus.Wherein the patient of 20%-25% is the cancer of the esophagus in early days, and its postoperative 5 years survival rates are about 50%;But for Locally Advanced (IIB phase and the III phase) patient of 75-80%, 5 years survival rates of surgery alone excision treatment are only 20.64~34.00%, and transfer or local recurrence occurs in most of patients Post operation in 3 years.Visible, the survival rate of IIB phase and III phase patient largely represents the effect of esophageal carcinoma therapy.So, improve the curative effect of the cancer of the esophagus, in addition to examining, early control morning, it is important to improve the cure rate of local advanced esophageal carcinoma.
Recent research shows, staging tomography or chemicotherapy (lower rectal cancer) the Therapeutic mode performed the operation can be effectively improved Locally Advanced 5 years survival rates of esophageal squamous cell carcinoma curative effect patient can bring up to more than 50%.But, there is heterogeneity in the curative effect reaction to lower rectal cancer for the esophageal squamous cell carcinoma.Even if applying identical chemotherapeutics and dosage, identical radiotherapy pattern and dosage treat the patient being in same clinical stages, pathology curative effect reaction difference.The Patients With Carcinoma of Esophagus that about 50%-60% accepts visiting before operation cannot benefit owing to chemicotherapy tolerates.Therefore, reduce the chemicotherapy tolerance of esophageal squamous cell carcinoma, be the key point improving the existence of Locally Advanced patients with esophageal squamous cell carcinoma.But there is no effective medicine and the using method thereof alleviating chemicotherapy tolerance at present.
Bcl-2 protein family is one group of key protein of regulating cell programmed death, and IAP (such as Bcl-2 albumen and Bcl-Xl albumen) and apoptosis can be divided into promote albumen (such as Bak albumen and Bax albumen) two classifications.The apoptosis such as Bak with Bax promote that the feature of albumen is to have the domain (BH3 domain) of a highly similar αhelix, this domain has the function of the IAPs such as suppression Bcl-2 and Bcl-Xl, thus inducing cell generating program is dead.4-[4-[(4'-chlorine [1,1'-biphenyl]-2-base) methyl]-1-piperazinyl]-N-[[4-[[(1R)-3-(dimethylamino)-1-[(thiophenyl) methyl] propyl group] amino]-3-nitrobenzophenone] sulfonyl] benzamide (chemical formula C42H45ClN6O5S2, code name ABT-737) and structure is similar to " the BH3 domain " of Bad albumen, can suppress Bcl-2, Bcl-Xl and Bcl-w albumen, and reduce Bcl-2 and BAX and form heterodimer, inducing cell apoptosis.ABT-737, main by the effective inducing cell apoptosis of two mechanism: (1) promotes Bax and Bak oligomerization and cromoci release;(2) be combined with anti-apoptotic proteins such as Bcl-2 and Bcl-Xl, reduce their inhibitory action to BH3 albumen.
Have been reported, in experiment in vitro, ABT-737 combined chemotherapy medicine also can increase ED-SCLC, filter blocking lymthoma, chronic lymphocytic leukemia, myeloma, colon cancer, breast cancer, Medulloblastoma, oophoroma to chemotherapeutics and (or) radioactive sensitiveness, promotion Apoptosis.But ABT-737 is not used for the treatment of the cancer of the esophagus so far, or ABT-737 combined chemotherapy medicine is used for strengthen the cancer of the esophagus to chemotherapeutics and (or) radioactive sensitiveness, raising esophageal carcinoma therapy effect.
Content of the invention
We have discovered that, Bcl-2/Bcl-Xl up-regulated in the cancer of the esophagus sample of tolerance in the chemotherapy based on cis-platinum, vinblastine and (or) radiotherapy, especially in the cancer of the esophagus that sodium hydrogen interchange channel albumen 9 (being called for short NHE9) protein expression raises, NHE9 is related to the rise of Bcl-2/Bcl-Xl;Apply ABT-737 combined chemotherapy and (or) radiotherapy in esophageal cancer cell, nude mice model, the sensitiveness to chemotherapy or radiotherapy for the cancer of the esophagus can be increased, improve esophageal carcinoma therapy effect.
A kind of medicine for treating the cancer of the esophagus of the present invention, it is characterised in that:
A, the described medicine for treating the cancer of the esophagus contain 4-[4-[(4'-chlorine [1,1'-biphenyl]-2-base) methyl]-1-piperazinyl]-N-[[4-[[(1R)-3-(dimethylamino)-1-[(thiophenyl) methyl] propyl group] amino]-3-nitrobenzophenone] sulfonyl] benzamide (chemical formula C42H45ClN6O5S2, code name ABT-737) or the compound with described ABT-737 as basic system;
B, the chemical formula of described ABT-737 be:
C, the described medicine for treating the cancer of the esophagus are for treating the cancer of the esophagus, or as Chemotherapy in Esophageal Cancer and radiocurable hypersitization medicine.
The described medicine for treating the cancer of the esophagus can be used in combination at least one course for the treatment of with the chemotherapeutics of the treatment cancer of the esophagus, including but not limited to cis-platinum, NVB.The chemotherapeutics of the present invention can be replaced by other chemotherapeutics with result for the treatment of, and such as taxol, gemcitabine, 5 FU 5 fluorouracil, endoxan etc., the chemotherapeutics of introduction simultaneously of the present invention not reaches unique medication of result for the treatment of.Those skilled in the art can make countless change, improvement and replacements in chemotherapeutics use, without departing from the present invention.
The described medicine for treating the cancer of the esophagus can use at least one course for the treatment of with the chemotherapy combined radiotherapy of the cancer of the esophagus.The described medicine for treating the cancer of the esophagus is recommended to be used in combination in each radiotherapy.Described ABT-737 can effectively reduce radiotherapy tolerance by suppression Bcl-2 and Bcl-Xl in each treatment, improves esophageal carcinoma therapy effect.
The described medicine for treating the cancer of the esophagus can use at least one course for the treatment of with the chemotherapy combined of the cancer of the esophagus.The described medicine for treating the cancer of the esophagus is recommended to be used in combination in each chemotherapy.Described ABT-737 can effectively reduce Chemoresistance by suppression Bcl-2 and Bcl-Xl in each treatment, improves esophageal carcinoma therapy effect.
The described medicine for treating the cancer of the esophagus can use at least one course for the treatment of with the chemoradiotherapy plus of the cancer of the esophagus.The described medicine for treating the cancer of the esophagus is recommended to be used in combination in each chemicotherapy.Described ABT-737 can effectively reduce chemicotherapy tolerance by suppression Bcl-2 and Bcl-Xl in each treatment, improves esophageal carcinoma therapy effect.
Further, during the described medicine for treating the cancer of the esophagus can be applicable to chemotherapy, radiotherapy or chemicotherapy;It is optimal to apply at the daystart accepting chemotherapy and radiation.The described medicine for treating the cancer of the esophagus of daystart application, can effectively suppress Bcl-2 and Bcl-Xl in early days, is conducive at utmost reducing tolerance, the maximum therapy effect playing medicine and radioactive ray.In human esophagus cancer nude mice knurl lotus model, use in first day of chemotherapy, radiotherapy or chemicotherapy treatment is effectively reduced the treatment tolerance of the cancer of the esophagus for the medicine treating the cancer of the esophagus, improves esophageal carcinoma therapy effect.
The dosage using in clinic of described ABT-737 contained in the described medicine for treating the cancer of the esophagus is 0.1mg/Kg~10.0mg/Kg, and optimal dose is 1.5mg/Kg~3.0mg/Kg.Experiment by human esophagus cancer nude mice knurl lotus model, the described ABT-737 of 20mg/Kg~30mg/Kg is effectively reduced chemotherapy, radiotherapy or chemicotherapy tolerance, according to U.S. FDA center for Drug Evaluation and Research (Center for Drug Evaluation and Research, CDER) humans and animals dose lonvestion guide, human administration's optimal dose is about 1.5mg/Kg~3.0mg/Kg.
The administering mode of the described medicine for treating the cancer of the esophagus includes intraperitoneal administration, intravenously administrable, intramuscular injection, is administered orally.It should be noted that administering mode disclosed and illustrated herein can be replaced by other administering modes with result for the treatment of, such as percutaneous dosing, endolumenal local administration etc., the administering mode of introduction simultaneously of the present invention not reaches the sole mode of result for the treatment of.Those skilled in the art can make countless change, improvement and replacements in terms of administering mode, without departing from the present invention.
The applicable crowd of the described medicine for treating the cancer of the esophagus can be defined by sodium hydrogen interchange channel albumen 9 (being called for short NHE9) expression.As shown in reference to Fig. 4, we have discovered that, when NHE9 up-regulated, Bcl-2 and Bcl-Xl related to the tolerance of Chemotherapy in Esophageal Cancer, radiotherapy or chemicotherapy expresses and also raises accordingly.And the present invention's is as Chemotherapy in Esophageal Cancer and radiocurable hypersitization medicine for one of important application of medicine treating the cancer of the esophagus, i.e. by suppressing the function of Bcl-2 and Bcl-Xl, reduce the tolerance to the chemotherapy of the cancer of the esophagus, radiotherapy or chemicotherapy for the patient and improve the result for the treatment of to the cancer of the esophagus.Therefore, the applicable crowd of the described medicine for treating the cancer of the esophagus can be bound by NHE9 expression.
The described medicine for treating the cancer of the esophagus is suitable for the positive cancer of the esophagus of NHE9 immunohistochemical staining, especially for the cancer of the esophagus more than 5 for the treatment NHE9 immunohistochemical staining scoring.We have discovered that, when NHE9 is the immunohistochemical staining positive, especially when immunohistochemical staining scoring is more than 5, there is tolerance possibility higher (P < 0.001) to the chemotherapy of the cancer of the esophagus, radiotherapy or chemicotherapy in patient, and detailed data is shown in Table 1.And the described medicine for treating the cancer of the esophagus is to improve the result for the treatment of to the cancer of the esophagus by reducing the tolerance to the chemotherapy of the cancer of the esophagus, radiotherapy or chemicotherapy for the patient, therefore, the described medicine for treating the cancer of the esophagus is suitable for treating the positive cancer of the esophagus of NHE9 immunohistochemical staining, the cancer of the esophagus positive especially for treatment NHE9, immunohistochemical staining scoring is more than 5.
The relation that table 1 NHE9 immunohistochemical staining level tolerates with esophageal carcinoma therapy
1 average age is 55 years old
2 mean body mass indices are 22.5
# Chi-square Test;* there is significant difference
A kind of medicine for treating the cancer of the esophagus of the present invention contains described ABT-737 or the compound with described ABT-737 as basic structure, is used for treating the cancer of the esophagus, or as Chemotherapy in Esophageal Cancer and radiocurable hypersitization medicine.A kind of medicine for treating the cancer of the esophagus of the present invention, by the mechanism of induced tumor apoptosis, reduces Chemotherapy in Esophageal Cancer and (or) radiotherapy tolerance, improves the result for the treatment of of the cancer of the esophagus, is conducive to improving patient with esophageal carcinoma cure rate and total existence.
Brief description
Figure 1A cancer of the esophagus immunohistochemical staining is negative.
The weak positive of Figure 1B cancer of the esophagus immunohistochemical staining.
Fig. 1 C cancer of the esophagus immunohistochemical staining moderate positive.
Fig. 1 D cancer of the esophagus immunohistochemical staining strong positive.
Fig. 1 E cancer of the esophagus immunohistochemical staining negative control.
Fig. 2 builds NHE9 process LAN or strikes fall cell line model.Wherein A is Western-blot detection process LAN or the result knocking out NHE9 protein expression situation in cell line;B is fluorescence quantitative PCR detection process LAN or the result knocking out NHE9 mRNA (mRNA) expression in cell line;C is the expression of Immunofluorescence test NHE9.
The impact on Radiotherapy of Esophageal Cancer, chemotherapy or Concurrent Chemoradiotherapy Sensitivity for Fig. 3 NHE9 high expressed.A is NHE9 process LAN or knocks out impact on Chemotherapy in Esophageal Cancer medicine IC50 dosage;B is NHE9 process LAN or knocks out impact on cancer of the esophagus radiation-sensitive.
The impact on Bcl-2/Bcl-Xl protein expression in the cancer of the esophagus after chemicotherapy process for Fig. 4 NHE9.
The sensitization to Chemotherapy in Esophageal Cancer tolerance in nude mice model for Fig. 5 ABT-737 combined chemotherapy.
The sensitization to Radiotherapy of Esophageal Cancer tolerance in nude mice model for Fig. 6 ABT-737 combined radiotherapy.
The sensitization to cancer of the esophagus chemicotherapy tolerance in nude mice model for Fig. 7 ABT-737 combined radio chemotherapy.
Detailed description of the invention
Experimental technique:
1st, it is estimated by the expression to NHE9 in the cancer of the esophagus for the immunohistochemical staining result
Method: after paraffin-embedded human esophageal carcinoma is sliced, immunohistochemical staining.Immunohistochemical staining result is divided into according to staining power: 0 point, dye-free;1 point, the weak positive;2 points, moderate positive;3 points, strong positive.It is divided into according to colored proportion: 0 point, < 5% positive cell;1 point, 5-25%;2 points, 26%-50%;3 points, 51%-75%;4 points, 76-100%.Two parts scoring is added, and obtaining immunohistochemical staining result is: 0-7 divides (with reference to Fig. 1).
2nd, build NHE9 process LAN or strike fall cell, animal model
The means utilizing molecular cloning build NHE9 and stablize process LAN or strike and slow down viral packaging plasmid, transfection 293FT cell produces slow virus, infect esophageal cancer cell strain, building NHE9 and stablizing process LAN esophageal squamous cell carcinoma cell KYSE30/NHE, Eca109/NHE and corresponding compared with control cells KYSE30/Con, Eca109/Con, NHE9 stably strikes fall esophageal squamous cell carcinoma cell KYSE180/sh1, KYSE180/sh2, KYSE520/sh1, KYSE520/sh2 and corresponding compared with control cells KYSE180/Con, KYSE520/Con.Cellar culture, in the DMEM culture medium containing 10%FBS, 100U/m1 penicillin and streptomysin, is placed in containing cultivation in 5%CO2,37 DEG C of incubator (with reference to Fig. 2).
Aforementioned stable process LAN NHE9 and comparison thereof or NHE9 express and stably knock out and the esophageal cancer cell strain of compared with control cells, are inoculated in 4-5 week nude mice back both sides.
3rd, the impact of the sensitiveness on Radiotherapy of Esophageal Cancer, chemotherapy or chemicotherapy for the NHE9 is detected
Detect the sensitiveness to chemotherapeutics for the cell with mtt assay, by the sensitiveness (with reference to Fig. 3) to radioactive ray for the colony formation detection cell.
Until transplanted tumor in nude mice grow naked eyes show when, select tumorous size consistent be randomly divided into experimental group, control group, experimental group lumbar injection gives chemotherapeutics: cis-platinum 4mg/kg+ vinorelbine 2mg/kg, 1 times a week, and (or) continuous 4 weeks, radioactive ray irradiate use RS-2000X x ray irradiation x instrument be irradiated, 6Gy/ time, 1 times a week, continuous 4 weeks;Using physiological saline group as blank group.Within every 3 days, weigh in 1 time, and the major diameter of tumour, minor axis, calculate gross tumor volume, draw tumor growth curve, observe chemotherapeutics and radioactive ray NHE9 process LAN or esophageal squamous cell carcinoma cell line transplanted tumor in nude mice growth inhibition effect that expression knocks out;Contrast experiment's group and control group gross tumor volume and weight.Kill mouse when blank group tumour is more than 1g, take tumour and weigh, calculate each group of tumour inhibiting rate.
4th, the impact that Bcl-2/Bcl-Xl after the process of chemotherapy, radiotherapy or chemicotherapy is expressed by NHE9 is detected
Collect chemotherapy, radiotherapy or chemicotherapy process after NHE9 process LAN or strike fall cell, the impact (reference Fig. 4) that Bcl-2/Bcl-Xl is expressed by Western blot checking NHE9.
Embodiment one: a kind of medication combined chemotherapy for treating the cancer of the esophagus of the present invention is for treating the cancer of the esophagus
In the present embodiment, the described medicine for treating the cancer of the esophagus is the hypersitization medicine as Chemotherapy in Esophageal Cancer, and chemotherapeutics is used in combination.
In the present embodiment; the described medicine for treating the cancer of the esophagus contains 4-[4-[(4'-chlorine [1,1'-biphenyl]-2-base) methyl]-1-piperazinyl]-N-[[4-[[(1R)-3-(dimethylamino)-1-[(thiophenyl) methyl] propyl group] amino]-3-nitrobenzophenone] sulfonyl] benzamide (chemical formula C42H45ClN6O5S2, code name ABT-737) and physiological saline, the concentration of described ABT-737 is 200mg/mL.
The chemical formula of described ABT-737 is:
In the present embodiment, first human esophagus cancer cell is inoculated in nude mice dorsal sc, builds human esophagus cancer nude mice knurl lotus model.Until tumour grow naked eyes show when, be randomly divided into experimental group, control group, control group lumbar injection gives chemotherapeutics: cis-platinum 4mg/kg+ vinorelbine 2mg/kg, 1 times a week, continuous 4 weeks;Experimental group abdominal cavity gives the chemotherapeutic of same dose and species, and abdominal cavity is given and ABT-737 simultaneously, according to reference dose 20mg/Kg, using physiological saline group as blank group.Within every 3 days, weigh in 1 time, calculate gross tumor volume, draw tumor growth curve, the esophageal squamous cell carcinoma cell line transplanted tumor in nude mice growth inhibition effect that observation chemotherapeutics and radioactive ray NHE9 process LAN or expression knock out;Contrast experiment's group and control group gross tumor volume and weight, analyze effect in NHE9 high expressed esophageal squamous cell carcinoma chemicotherapy for the ABT-737.When blank group tumour is more than 1g, takes tumour and calculate each group of tumour inhibiting rate.
As shown in reference to Fig. 5, through statistical analysis, it is 1427.2 ± 152.4mm that the control group NHE9 high expressed cancer of the esophagus becomes knurl volume3, it is 808.3 ± 117.6mm that the non-NHE9 high expressed cancer of the esophagus becomes knurl volume3, therefore, NHE9 high expressed has notable significant difference (P=0.005) with the knurl volume that becomes of the non-NHE9 high expressed cancer of the esophagus.It is 956.4 ± 242.7mm that the experimental group NHE9 high expressed cancer of the esophagus becomes knurl volume3, the non-NHE9 high expressed cancer of the esophagus becomes knurl volume 657.8 ± 205.1mm3, NHE9 high expressed becomes knurl volume without obvious significant difference (P=0.35) with the non-NHE9 high expressed cancer of the esophagus.
It can be seen that the NHE9 high expressed cancer of the esophagus demonstrates Chemoresistance from Data Comparison, the non-NHE9 high expressed cancer of the esophagus does not shows tolerance to chemotherapeutics.When do not use the present invention for treating the medicine of the cancer of the esophagus when, when the cancer of the esophagus shows tolerance to chemotherapeutics, the cancer of the esophagus becomes knurl volume (1427.2 ± 152.4mm3) substantially than non-tolerance when become knurl volume (808.3 ± 117.6mm3) big, knurl volume notable difference (P=0.005) occurs, illustrate, when chemotherapeutics is occurred tolerating by the NHE9 high expressed cancer of the esophagus, the result for the treatment of of chemotherapeutics is poor.And when when being used for the medicine treating the cancer of the esophagus of the use present invention, even NHE9 high expressed, when i.e. the cancer of the esophagus shows tolerance to chemotherapeutics, the one-tenth knurl volume (956.4 ± 242.7mm of the cancer of the esophagus3) with do not use the present invention for treating the medicine of the cancer of the esophagus when become knurl volume (1427.2 ± 152.4mm3) compare and occur in that and be decreased obviously, and the tolerance cancer of the esophagus non-with chemotherapy become knurl volume (657.8 ± 205.1mm3) no significant difference (P=0.35).This proves, the present invention can substantially reduce the tolerance to chemotherapeutics for the NHE9 high expressed cancer of the esophagus for the medicine treating the cancer of the esophagus, thus improves the result for the treatment of to the cancer of the esophagus.
According to U.S. FDA center for Drug Evaluation and Research (Center for Drug Evaluation and Research, CDER) humans and animals dose lonvestion guide, reduction formula is as follows:
The Km coefficient of the Km coefficient/animal A of animal A (mg/kg)=animal B (mg/kg) × animal B
Mouse Km coefficient is 3, and adult's Km coefficient term of reference is 30~40, brings formula into and calculates, and human administration's optimal dose is about 1.5mg/Kg~3.0mg/Kg.
During Clinical practice, the described medicine for treating the cancer of the esophagus is liquid injection, chemotherapy the 1st day, by the described clinical dosage being used for treating the medicine of the cancer of the esophagus by way of drip-feed, and pressing 1.5mg/Kg~3.0mg/Kg, is administered.
The described medicine for treating the cancer of the esophagus and chemotherapeutic drugs Cisplatin, NVB are used in combination 2 courses for the treatment of altogether.
A kind of medicine for treating the cancer of the esophagus of the present invention contains described ABT-737, can be as the hypersitization medicine of Chemotherapy in Esophageal Cancer.A kind of medicine for treating the cancer of the esophagus of the present invention, by the mechanism of induced tumor apoptosis, reduces the tolerance of Chemotherapy in Esophageal Cancer, can improve the result for the treatment of of the cancer of the esophagus, is conducive to improving patient with esophageal carcinoma cure rate and total existence.
Embodiment two: a kind of medication combined radiotherapy for treating the cancer of the esophagus of the present invention substantially increases the sensitiveness to treatment for the cancer of the esophagus
The present embodiment is with the difference of embodiment one, and the medicine being used for treating the cancer of the esophagus described in the present embodiment is the hypersitization medicine as radiotherapy for esophageal carcinoma, and radiotherapy is used in combination.
The control group radioactive ray irradiate and use RS-2000X x ray irradiation x instrument to be irradiated, 6Gy/ time, 1 times a week, and continuous 4 weeks;Experimental group equivalent radio exposure abdominal cavity simultaneously is given and ABT-737.
As shown in reference to Fig. 6, through statistical analysis, it is 1324.7 ± 143.3mm that the control group NHE9 high expressed cancer of the esophagus becomes knurl volume3, it is 578.6 ± 237.1mm that the non-NHE9 high expressed cancer of the esophagus becomes knurl volume3, therefore, NHE9 high expressed has notable significant difference (P=0.005) with the knurl volume that becomes of the non-NHE9 high expressed cancer of the esophagus.It is 922.2 ± 119.2mm that the experimental group NHE9 high expressed cancer of the esophagus becomes knurl volume3, the non-NHE9 high expressed cancer of the esophagus becomes knurl volume 623.9 ± 303.1mm3, NHE9 high expressed becomes knurl volume without obvious significant difference (P=0.35) with the non-NHE9 high expressed cancer of the esophagus.
It can be seen that the NHE9 high expressed cancer of the esophagus demonstrates Chemoresistance from Data Comparison, the non-NHE9 high expressed cancer of the esophagus does not shows tolerance to chemotherapeutics.When do not use the present invention for treating the medicine of the cancer of the esophagus when, when the cancer of the esophagus shows tolerance to chemotherapeutics, the cancer of the esophagus becomes knurl volume (1324.7 ± 143.3mm3) substantially than non-tolerance when become knurl volume (578.6 ± 237.1mm3) big, knurl volume notable difference (P=0.005) occurs, illustrate, when chemotherapeutics is occurred tolerating by the NHE9 high expressed cancer of the esophagus, the result for the treatment of of chemotherapeutics is poor.And when when being used for the medicine treating the cancer of the esophagus of the use present invention, even NHE9 high expressed, when i.e. the cancer of the esophagus shows tolerance to chemotherapeutics, the one-tenth knurl volume (922.2 ± 119.2mm of the cancer of the esophagus3) with do not use the present invention for treating the medicine of the cancer of the esophagus when become knurl volume (1324.7 ± 143.3mm3) compare and occur in that and be decreased obviously, and the tolerance cancer of the esophagus non-with chemotherapy become knurl volume (623.9 ± 303.1mm3) no significant difference (P=0.35).This proves, the present invention can substantially reduce the tolerance to chemotherapeutics for the NHE9 high expressed cancer of the esophagus for the medicine treating the cancer of the esophagus, thus improves the result for the treatment of to the cancer of the esophagus.
According to U.S. FDA center for Drug Evaluation and Research (Center for Drug Evaluation and Research, CDER) humans and animals dose lonvestion guide, reduction formula is as follows:
The Km coefficient of the Km coefficient/animal A of animal A (mg/kg)=animal B (mg/kg) × animal B
Mouse Km coefficient is 3, and adult's Km coefficient term of reference is 30~40, brings formula into and calculates, and human administration's optimal dose is about 1.5mg/Kg~3.0mg/Kg.
During Clinical practice, the described medicine for treating the cancer of the esophagus is liquid injection, radiotherapy the 1st day, by the described clinical dosage being used for treating the medicine of the cancer of the esophagus by way of drip-feed, and pressing 1.5mg/Kg~3.0mg/Kg, is administered.
The described medicine for treating the cancer of the esophagus and chemotherapy combined radiotherapy use and amount to 2 courses for the treatment of.
A kind of medicine for treating the cancer of the esophagus of the present invention contains described ABT-737, can be as the hypersitization medicine of Radiotherapy of Esophageal Cancer.A kind of medicine for treating the cancer of the esophagus of the present invention, by the mechanism of induced tumor apoptosis, reduces the tolerance of Radiotherapy of Esophageal Cancer, can improve the result for the treatment of of the cancer of the esophagus, is conducive to improving patient with esophageal carcinoma cure rate and total existence.
Embodiment three: a kind of medication combined chemicotherapy for treating the cancer of the esophagus of the present invention substantially increases the sensitiveness to treatment for the cancer of the esophagus
The present embodiment is with the difference of embodiment one, and the medicine being used for treating the cancer of the esophagus described in the present embodiment is the hypersitization medicine as cancer of the esophagus chemicotherapy, and chemicotherapy is used in combination.
As shown in reference to Fig. 7, through statistical analysis, it is 1138.1 ± 91.8mm that the control group NHE9 high expressed cancer of the esophagus becomes knurl volume3, it is 520.3 ± 242.9mm that the non-NHE9 high expressed cancer of the esophagus becomes knurl volume3, therefore, NHE9 high expressed has notable significant difference (P=0.02) with the knurl volume that becomes of the non-NHE9 high expressed cancer of the esophagus.It is 610.8 ± 184.3mm that the experimental group NHE9 high expressed cancer of the esophagus becomes knurl volume3, the non-NHE9 high expressed cancer of the esophagus becomes knurl volume 412.5 ± 223.5mm3, NHE9 high expressed becomes knurl volume without obvious significant difference (P=0.12) with the non-NHE9 high expressed cancer of the esophagus.
It can be seen that the NHE9 high expressed cancer of the esophagus demonstrates Chemoresistance from Data Comparison, the non-NHE9 high expressed cancer of the esophagus does not shows tolerance to chemotherapeutics.When do not use the present invention for treating the medicine of the cancer of the esophagus when, when the cancer of the esophagus shows tolerance to chemotherapeutics, the cancer of the esophagus becomes knurl volume (1138.1 ± 91.8mm3) substantially than non-tolerance when become knurl volume (520.3 ± 242.9mm3) big, knurl volume notable difference (P=0.02) occurs, illustrate, when chemotherapeutics is occurred tolerating by the NHE9 high expressed cancer of the esophagus, the result for the treatment of of chemotherapeutics is poor.And when when being used for the medicine treating the cancer of the esophagus of the use present invention, even NHE9 high expressed, when i.e. the cancer of the esophagus shows tolerance to chemotherapeutics, the one-tenth knurl volume (610.8 ± 184.3mm of the cancer of the esophagus3) with do not use the present invention for treating the medicine of the cancer of the esophagus when become knurl volume (1138.1 ± 91.8mm3) compare and occur in that and be decreased obviously, and the tolerance cancer of the esophagus non-with chemotherapy become knurl volume (412.5 ± 223.5mm3) no significant difference (P=0.12).This proves, the present invention can substantially reduce the tolerance to chemotherapeutics for the NHE9 high expressed cancer of the esophagus for the medicine treating the cancer of the esophagus, thus improves the result for the treatment of to the cancer of the esophagus.
According to U.S. FDA center for Drug Evaluation and Research (Center for Drug Evaluation and Research, CDER) humans and animals dose lonvestion guide, reduction formula is as follows:
The Km coefficient of the Km coefficient/animal A of animal A (mg/kg)=animal B (mg/kg) × animal B
Mouse Km coefficient is 3, and adult's Km coefficient term of reference is 30~40, brings formula into and calculates, and human administration's optimal dose is about 1.5mg/Kg~3.0mg/Kg.
During Clinical practice, the described medicine for treating the cancer of the esophagus is liquid injection, chemicotherapy the 1st day, by the described clinical dosage being used for treating the medicine of the cancer of the esophagus by way of drip-feed, and pressing 1.5mg/Kg~3.0mg/Kg, is administered.
The described medicine for treating the cancer of the esophagus and chemoradiotherapy plus use and amount to 2 courses for the treatment of.
A kind of medicine for treating the cancer of the esophagus of the present invention contains described ABT-737, can be as the hypersitization medicine of cancer of the esophagus chemicotherapy.A kind of medicine for treating the cancer of the esophagus of the present invention, by the mechanism of induced tumor apoptosis, reduces the tolerance of cancer of the esophagus chemicotherapy, can improve the result for the treatment of of the cancer of the esophagus, is conducive to improving patient with esophageal carcinoma cure rate and total existence.
It should be noted that medicine disclosed and illustrated herein and using method thereof can be with the identical compounds of other active ingredients, the embodiment that the present invention is introduced simultaneously not realizes the unique method of the present invention.Although the preferred embodiments of the present invention is introduced herein and is illustrated; but those skilled in the art are aware that and know that these embodiments are only to illustrate; those skilled in the art can make countless change, improvement and replacements; without departing from the present invention; therefore, protection scope of the present invention should be limited according to the spirit and scope of claims appended hereto.

Claims (9)

1. the medicine being used for treating the cancer of the esophagus, it is characterised in that:
A, the described medicine for treating the cancer of the esophagus [4-[(4'-chlorine [1,1'-biphenyl]-2-base) the methyl]-1-piperazine containing 4- Base]-N-[[4-[[(1R)-3-(dimethylamino)-1-[(thiophenyl) methyl] propyl group] amino]-3-nitrobenzophenone] sulfonyl] benzamide (chemical formula C42H45ClN6O5S2, code name ABT-737) or the compound with described ABT-737 as basic system;
B, the chemical formula of described ABT-737 be:
C, the described medicine for treating the cancer of the esophagus for treating the cancer of the esophagus, or as cancer of the esophagus chemotherapy (chemotherapy) and The hypersitization medicine of radiotherapy (radiotherapy).
2. according to claim 1 for treating the medicine of the cancer of the esophagus, it is characterised in that: described for treating the cancer of the esophagus Medicine can be used in combination at least one with the chemotherapeutics of the treatment cancer of the esophagus, including but not limited to cis-platinum, NVB The individual course for the treatment of.
3. according to claim 1 for treating the medicine of the cancer of the esophagus, it is characterised in that: described for treating the cancer of the esophagus Medicine can be used in combination at least one course for the treatment of with the radiotherapy of the cancer of the esophagus.
4. according to claim 1 for treating the medicine of the cancer of the esophagus, it is characterised in that: described for treating the cancer of the esophagus Medicine can be used in combination at least one course for the treatment of with the radiation and chemotherapy of the cancer of the esophagus.
5. according to claim 1 for treating the medicine of the cancer of the esophagus, it is characterised in that: described for treating the cancer of the esophagus Medicine can be applicable to chemotherapy, radiotherapy or radiotherapy associating chemotherapy (chemicotherapy) period;To accept chemotherapy or radiotherapy Daystart application be optimal.
6. according to claim 1 for treating the medicine of the cancer of the esophagus, it is characterised in that: described for treating the cancer of the esophagus The dosage using in clinic of described ABT-737 contained in medicine is 0.1mg/Kg~10.0mg/Kg, and optimal dose is 1.5mg/Kg~3.0mg/Kg.
7. according to claim 1 for treating the medicine of the cancer of the esophagus, it is characterised in that: described for treating the cancer of the esophagus The administering mode of medicine includes intraperitoneal administration, intravenously administrable, intramuscular injection, is administered orally.
8. according to claim 1 for treating the medicine of the cancer of the esophagus, it is characterised in that: described for treating the cancer of the esophagus The applicable crowd of medicine can be defined by sodium hydrogen interchange channel 9 albumen (being called for short NHE9) expression.
9. according to claim 8 for treating the medicine of the cancer of the esophagus, it is characterised in that: described for treating the cancer of the esophagus Medicine is applicable to the positive cancer of the esophagus of NHE9, big especially for the treatment NHE9 positive, immunohistochemical staining index In the patient with esophageal carcinoma of 5.
CN201510205305.0A 2015-04-27 2015-04-27 A kind of medicine for treating the cancer of the esophagus and using method Pending CN106074574A (en)

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Cited By (1)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
WO2022105511A1 (en) * 2020-11-19 2022-05-27 苏州正永生物医药有限公司 Use of bcl-2 inhibitor and pharmaceutical composition for treating aging-related skin disease

Non-Patent Citations (1)

* Cited by examiner, † Cited by third party
Title
JUNYING CHEN ETAL: "NHE9 induces chemoradiotherapy resistance in esophageal squamous cell carcinoma by upregulating the Src/Akt/β-catenin pathway and Bcl-2 expression", 《ONCOTARGET.》 *

Cited By (1)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
WO2022105511A1 (en) * 2020-11-19 2022-05-27 苏州正永生物医药有限公司 Use of bcl-2 inhibitor and pharmaceutical composition for treating aging-related skin disease

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Application publication date: 20161109