CN102396476A - Murine sterilant bait for controlling rodent damage in farmland and grassland - Google Patents
Murine sterilant bait for controlling rodent damage in farmland and grassland Download PDFInfo
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- CN102396476A CN102396476A CN2010102795471A CN201010279547A CN102396476A CN 102396476 A CN102396476 A CN 102396476A CN 2010102795471 A CN2010102795471 A CN 2010102795471A CN 201010279547 A CN201010279547 A CN 201010279547A CN 102396476 A CN102396476 A CN 102396476A
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Abstract
The invention discloses a murine sterilant bait and a preparation method thereof. The murine sterilant bait comprises a basic bait, a warning color and the original drug of a sterilant, wherein, the basic bait comprises 10 to 30% of corn grit, 10 to 30% of naked oat powder, 60% of dry grass meal and 0.5 to 0.7% of peanut oil. According to the invention, dry grass meal and naked oat flour are targetedly added into the murine sterilant bait; a formula for the murine sterilant bait is reasonable, materials to prepare the murine sterilant bait are easily available, and it is convenient to prepare and utilize the murine sterilant bait; an fertility control effect on bandicoots in farmland and grassland is improved; palatability of the bait is good, the intake rate of bandicoots is increased, while intake of the bait by other animals is effectively avoided, and therefore, the bait has the advantage of environmental security.
Description
Technical field
The present invention relates to a kind of rodents sterilant pharmaceutical chemistry that is used to prevent and treat grassland, the farmland plague of rats.
Background technology
Sterile control is to prevent and treat one of new technology of grassland, the farmland plague of rats in recent years, have pollution-free, the lasting period long, advantage such as inexpensive.In implementation process, make muroid can eat the pharmaceutical chemistry of capacity and guarantee that non-target animal does not eat or the medicine for lack of appetite bait is the major issue that guarantees control effect and human and environment safety.
The common prescription of rodenticide pharmaceutical chemistry that uses at the control plague of rats is: medicine+basic bait (like corn, wheat or paddy)+warning colouration+clear water.Its advantage is that raw material is easy to get, and preparing process is simple.But shortcoming is to be easy to searched for food by insects such as non-target animal, particularly domestic animal, granivores and ants.Both cause the waste of pharmaceutical chemistry, also can accidentally injure non-target animal.
Solve pharmaceutical chemistry to the palatability of muroid and to avoid non-target animal to eat by mistake be one of technology that the various countries scientist makes great efforts to explore in the rat plague control.As adopt in wax bait (like German BASF AG) or the pharmaceutical chemistry measures such as adding bitters, (like the bitters ratsbane patent publication No. CN 1778178A of Yuan Guangming (2006) invention).
Li Bos etc. (2007) have invented control and have hidden the apholate poison bait (patent publication No. CN 101023745A) that northern Ochotona curzoniae poison bait and preparation method are applicable to Ochotona curzoniae.But the problem that all unresolved wild birds of these pharmaceutical chemistry is eaten by mistake.
Administer the reality of the important channel of the plague of rats in view of sterile control in recent years through becoming the grassland, farmland, disposing a kind of efficient, safe, practical pharmaceutical chemistry has become vast scientific research and has put into practice worker's active demand.Under the pressure of the needs of grain security, prescription bait has become the carrier that replaces single cereal gradually and become the finished product rat-bane.
Summary of the invention
The purpose of this invention is to provide a kind of rodents sterilant pharmaceutical chemistry that is used to prevent and treat grassland, the farmland plague of rats and preparation method thereof.
The rodents sterilant pharmaceutical chemistry that the present invention is prepared comprises the former medicine component of basic bait, warning colouration and apholate;
Wherein, basic bait is made up of following component:
Maize pulp or ground rice 10~30%;
Grass meal 55-60%;
Peanut oil 0.5~0.7%.
Base bait component preferably is made up of following component:
Maize pulp or ground rice 10~29.5%;
Hay meal 60%;
Peanut oil 0.5~0.7%;
Said basic bait component most preferably is following 1)-3) in any described component:
1) form by following component:
Maize pulp 29.5%;
Hay meal 60%;
Peanut oil 0.5%;
2) form by following component:
Naked oats flour 29.3%;
Hay meal 60%;
Peanut oil 0.7%;
3) form by following component:
Naked oats flour 29.3%;
Hay meal 60%;
Peanut oil 0.7%.
Said warning colouration is edible light blue, and its addition is 0.01% of a said basic bait constituent mass.
The former medicine of apholate is that quinestrol and Levonorgestrel are mixing in 1: 2 according to weight ratio, and the addition of the former medicine of apholate is 0.005% of a said basic bait constituent mass.
Above-mentioned percentage composition is the quality percentage composition.
Said grass meal is feed market Powdered herbage commonly used, specifically can be the Powdered grass meal of daghestan sweet clover or sheep's hay, clover modulation.
Said rodents sterilant pharmaceutical chemistry is rolling growth 8-15mm, the cylindrical particle of the about 2-3mm of diameter.
In the above-mentioned rodents sterilant pharmaceutical chemistry, when using maize pulp, be applicable to and prevent and treat the northern China bandicoot that maize pulp is meant the maize pulp (small rice grain size) that iblet forms through roughing here.When using ground rice, be applicable to that ground rice refers to make and fry the used raw material of powder with long-grained nonglutinous rice processing here in China south.Southern and northern boundary is roughly the Qinling Mountains-Huaihe River.
The preparation method of above-mentioned rodents sterilant pharmaceutical chemistry comprises the steps:
(1) the former medicine of apholate is mixed with peanut oil, container is placed 40-60 ℃ of water-bath 40min, and constantly stir and make it dissolving and obtain original liquid;
(2) the good original liquid of (1) dissolving is poured in the naked oats flour and is fully stirred soup is uniformly dispersed, during add warning colouration and stir, be made into female powder I;
(3) the female powder I that (2) is made into fully mixes with maize pulp or rice ground rice, stirs with agitator to make it to mix, and is made into female powder II;
(4) the female powder II that (3) is made into mixes with hay meal, stirs, and is made into the pharmaceutical chemistry powder;
(5) the pharmaceutical chemistry powder that (4) is made into mixes after the proper amount of clear water at the rolling growth 8~15mm of granule, and the cylindrical particle of the about 3mm of diameter, natural air drying obtain the rodents sterilant pharmaceutical chemistry;
Each component is added according to above-mentioned content ratio.
Rodents sterilant pharmaceutical chemistry provided by the invention is that the compound apholate compatibility typical case of a kind of steroids bait forms, and belongs to chemical pharmaceutical chemistry.It has following characteristics with respect to prior art:
(1) adds peanut oil, naked oats face and grass meal in the bait and increased the palatability of muroid and the degree of packing of particle.
(2) bait formula is simple, and raw material is common to be easy to get, and saves grain.
(3) bait is pressed into long column strip particle bait grain, effectively avoids eating by mistake of non-target animal, and got food residue pharmaceutical chemistry by muroid and be easy to decompose, have environmental safety.
(4) the former medicine in bait compacting back is in the dry carrier, and drug effect can keep (term of validity 3 years) for a long time.
(5) fully be blended in all particles of bait owing to medicine; Each mouthful that muroid is eaten into all contains the identical medicine of concentration; Thereby only more meet the rodent foraging habit attached to the wheat surface with its medicine of pharmaceutical chemistry of traditional wheat configuration, can guarantee that medicine can play one's part to the full.
(6) use safety is because the hidden danger that the warning colouration effect can effectively avoid the bait grain to give domestic animal as the normal diet mistake.
(7) to dispensing person's safety, it is dangerous not have contamination.
The present invention is mixed with the sterile bait with special component first, adds the danger that 60% grass meal and warning colouration have not only increased the muroid palatability but also can avoid people and animals to eat by mistake, also can avoid non-target animal (particularly wild birds and carnivore) to eat effectively.And the shape of pharmaceutical chemistry is easy to mechanization bait throwing in operation; Using every of space China board suspension type strength spraying machine working area in the Erdos is 5000~6000 mu/day.Field trial proves; This pharmaceutical chemistry prescription is reasonable, and this pharmaceutical chemistry material obtains configuration technology and easy to use easily; Not only improved sterile control effect to grassland, farmland bandicoot; And this pharmaceutical chemistry is good to the muroid palatability, in the grazing rate that improves bandicoot, can effectively avoid the food of getting of non-target animal, therefore also has environmental safety.
Below in conjunction with accompanying drawing and embodiment the present invention is described further
Embodiment
Experimental technique described in the following embodiment like no specified otherwise, is conventional method.
Percentage composition described in the following embodiment is the quality percentage composition.
The preparation of embodiment 1, rodents sterilant pharmaceutical chemistry of the present invention
(1) rodents sterilant pharmaceutical chemistry of the present invention comprises the former medicine component of basic bait component, warning colouration and apholate;
Base bait component is made up of following component:
Maize pulp 29.5%;
Hay meal (with daghestan sweet clover or sheep's hay or clover air-dry then roll form) 60%;
Peanut oil 0.5%;
Warning colouration is edible light blue, and its addition is 0.01% of an above-mentioned basic bait constituent mass; Maize pulp is meant the maize pulp (small rice grain size) that iblet forms through roughing.
The former medicine of apholate is that quinestrol and Levonorgestrel are mixing in 1: 2 according to weight ratio, and the addition of the former medicine of apholate is 0.005% of an above-mentioned basic bait constituent mass.
(2) concrete grammar of preparation 1000kg rodents sterilant pharmaceutical chemistry is described below:
(1) the former medicine 50g of apholate (quinestrol 16.7g, Levonorgestrel 33.3g) is added 5kg peanut oil and pour in the container, container is placed 60 ℃ of water-bath 40min, and constantly stirring makes it to form the suspension soup;
(2) the good former medicine of (1) dissolving is poised liquid and add to pour in the 100kg naked oats flour and fully behind the edible light blue of 100g and stir, be made into female powder I;
(3) the female powder I that (2) is made into fully mixes with the 295kg maize pulp, stirs with agitator, is made into female powder II;
(4) the female powder II and the 600kg grass meal (the daghestan sweet clover hay meal is available from poultry sunlight company in the Chinese Academy of Agricultural Sciences) that (3) are made into fully mix, and stir with agitator, are made into the pharmaceutical chemistry powder;
(5) the pharmaceutical chemistry powder that (4) is made into mixes after the proper amount of clear water at the rolling growth 8-15mm of granulator, and the cylindrical particle of the about 3mm of diameter, natural air drying obtain rodents sterilant pharmaceutical chemistry (as shown in Figure 1).
The preparation of embodiment 2, rodents sterilant pharmaceutical chemistry of the present invention
(1) rodents sterilant pharmaceutical chemistry of the present invention comprises the former medicine component of basic bait component, warning colouration and apholate;
Base bait component is made up of following component:
Naked oats flour 29.3%;
Hay meal (with daghestan sweet clover or sheep's hay or clover air-dry then roll form) 60%;
Peanut oil 0.7%;
Warning colouration is edible light blue, and its addition is 0.01% of an above-mentioned basic bait constituent mass; Maize pulp is meant the maize pulp (small rice grain size) that iblet forms through roughing.
The former medicine of apholate is that quinestrol and Levonorgestrel are mixing in 1: 2 according to weight ratio, and the addition of the former medicine of apholate is 0.005% of an above-mentioned basic bait constituent mass.
2, the concrete grammar of preparation 1000kg rodents sterilant pharmaceutical chemistry is described below:
(1) the former medicine 50g of apholate (quinestrol 16.7g+ Levonorgestrel 33.3g) is poured in the container of the peanut oil that fills 7kg, container is placed 40 ℃ of water-bath 40min, and constantly stirring makes it to form the suspension soup;
(2) the good former medicine of (1) dissolving is poised liquid and add to pour in the 293kg naked oats flour and fully behind the edible light blue of 100g and stir, be made into female powder I;
(3) the female powder I that (2) is made into fully mixes with 100kg maize pulp (small rice grain size), stirs with agitator, is made into female powder II;
(4) the female powder II and the 600kg grass meal (sheep's hay hay meal, poultry sunlight company in the Chinese Academy of Agricultural Sciences) that (3) are made into fully mix, and stir with agitator, are made into the pharmaceutical chemistry powder;
(5) the pharmaceutical chemistry powder that (4) is made into mixes after the proper amount of clear water at the rolling growth 8-15mm of granule, and the cylindrical particle of the about 3mm of diameter, natural air drying obtain rodents sterilant pharmaceutical chemistry (as shown in Figure 1).
The preparation of embodiment 3, rodents sterilant pharmaceutical chemistry of the present invention
(1) rodents sterilant pharmaceutical chemistry of the present invention comprises the former medicine component of basic bait component, warning colouration and apholate;
Base bait component is made up of following component:
Naked oats flour 29.3%;
Hay meal (with daghestan sweet clover or sheep's hay or clover air-dry then roll form) 60%;
Peanut oil 0.7%;
Warning colouration is edible light blue, and its addition is 0.01% of an above-mentioned basic bait constituent mass;
The former medicine of apholate is that quinestrol and Levonorgestrel are mixing in 1: 2 according to weight ratio, and the addition of the former medicine of apholate is 0.005% of an above-mentioned basic bait constituent mass.
(2) concrete grammar of preparation 1000kg rodents sterilant pharmaceutical chemistry is described below:
(1) in the container of the former medicine 50g of apholate (quinestrol 16.7g+ Levonorgestrel 33.3g) and 7kg peanut oil being poured into, container is placed 40 ℃ of water-bath 40min, and constantly stir and make it to form the suspension soup;
(2) the good former medicine of (1) dissolving is poised liquid and add to pour in the 293kg naked oats flour and fully behind the edible light blue of 100g and stir, be made into female powder I;
(3) female powder I that (2) is made into and 100kg ground rice (the long-grained nonglutinous rice powder is done the raw material of frying powder, available from the luxuriant auspicious commerce and trade of standing grain in Beijing Co., Ltd) fully mix, and stir with agitator, are made into female powder II;
(4) the female powder II and the 600kg grass meal (alfalfa meal is available from poultry sunlight company in the Chinese Academy of Agricultural Sciences) that (3) are made into fully mix, and stir with agitator, are made into the pharmaceutical chemistry powder;
(5) the pharmaceutical chemistry powder that (4) is made into mixes after the proper amount of clear water at the rolling growth 8-15mm of granule, and the cylindrical particle of the about 3mm of diameter, natural air drying obtain rodents sterilant pharmaceutical chemistry (as shown in Figure 1).
The effect experiment of embodiment 4, rodents sterilant pharmaceutical chemistry of the present invention
Choose 40 of female adult meriones unguiculatuss, be divided into two groups (experimental group and control group, 10 every group) at random, feed the respectively rodents sterilant pharmaceutical chemistry of embodiment 1-embodiment 3 preparation of experimental group, control group fed corn particle.Indoor test, all test mouse are independent raising.
Duration of test, experimental group are raised with the rodents sterilant pharmaceutical chemistry; Control group is raised with iblet and was fed continuously for 1 week.
Test period is distinguished the consumption of weighing pharmaceutical chemistry and corn particle day by day.The result shows: the pharmaceutical chemistry day's expenditure of experimental group embodiment 1 preparation in preceding 3 days is 3.13g, a little less than the 3.34g of control group; The consumption of the pharmaceutical chemistry experimental group of embodiment 1 preparation thereafter increases gradually, to off-test.The pharmaceutical chemistry experimental group average daily consumed amt of embodiment 1 preparation is the 5.2g/ mouse, is significantly higher than the 4.8g/ mouse of control group, explains that the palatability of pharmaceutical chemistry is superior to corn.
The back measured with reproductive organs the hormone of experimental group mouse and showed administration 1 week, and the rodents sterilant pharmaceutical chemistry that this embodiment 1-embodiment 3 prepares can cause all that luteotropin and progesterone level obviously reduce in the female mouse blood; Internal organs are measured and are shown test mouse ovarian atrophy, and ovum arrest of development and part atrophy can not generate corpus luteum; Oedema appears in the uterus, and post-coitum embryo abnormal rate significantly improves; Match that reproduction rate is 0 in back 40 days.
The effect test of the rodents sterilant pharmaceutical chemistry that embodiment 5, instance of the present invention are prepared
In the laboratory, choose 40 of the male meriones unguiculatuss of adult; Be divided into 4 groups of (3 administration groups and 1 control group at random; Every group 10); The administration group is fed respectively one week of pharmaceutical chemistry that embodiment 1-embodiment 3 prepares continuously, and control group is fed simultaneously, and corn particle weighs, cuts open the seizure test group after 7 days and control group tries mouse, result such as following table (table 1)
Table 1 administration group and control group organ coefficient
Can find out that from table 1 the medication group is compared with control group, testis, epididymis, seminal vesicle organ coefficient significantly reduce, and reduce the most remarkable with instance 1.The medication group is bigger than the organ coefficient of control group spleen, increase with instance 1 the most remarkable, medication be described after, examination mouse immune burden increases the weight of, and causes spleen to increase weight, and has also embodied the action effect of medicine.
Can find out that from table 2 the medication group is compared sperm concentration with control group and obviously reduced, reduce the most obvious with instance 1 administration group density.
Table 2 different disposal sperm concentration relatively
| Group | Sperm concentration (individual/ml) |
| |
294.5×10 2 |
| |
330.6×10 2 |
| |
411.5×10 2 |
| Control group | 653×10 2 |
Can find out after the administration body weight of meriones unguiculatus not to be had tangible influence from table 3, other ill symptomses also not occur.Explain that sterile pharmaceutical chemistry does not influence examination mouse normal growth and grows.
Table 3 meriones unguiculatus different phase weight ratio
The field effect test of instance 6 rodents sterilant pharmaceutical chemistry of the present invention
In mid-March, 2009, Hangjin Banner Yi Ke Usu bush was chosen 0.75 hectare on appearance ground in Erdos, Inner Mongolia Autonomous Region, threw the every hole dispensing of the rodents sterilant pharmaceutical chemistry 5g of embodiment 1 preparation by the hole.Offer medicine after one month, in mid-April, 2009 all holes in appearance ground lay the mousetrap, caught and killed continuously 3 days.Investigation meriones unguiculatus breeding situation is analyzed drug effect; The place that is separated by beyond simultaneously on appearance ground more than 500 meters selects 0.75 hectare of kind of ground as contrast, with identical method investigation.Its result such as table 4, table 5.
The result shows: after 1 month, male mouse testis rate of descent reduction-dispensing district is 65.38% at medicine feed, and the check plot is 80%; Testicular volume and weight slightly reduce, and obvious atrophy takes place seminal vesicle.Influence to female mouse is: vaginal opening rate and pregnancy rate dispensing district are a little more than the check plot; And average tire newborn mouse dispensing Qu Zeyao is lower than the check plot; And still birth rate (80%) dispensing district is significantly higher than check plot (0), explains that this pharmaceutical chemistry has significant drug effect equally to male mouse and female mouse.Not only can make male mouse organ of multiplication damage but also can cause female mouse infertile.Female mouse shows as pregnancy rate and descends, and reduces even litter size also can appear in conceived female mouse, even directly causes stillborn foetus.
Table 4 dispensing is dispensing district and the male meriones unguiculatus investigation in check plot after 1 month
★ representes independent sample T test to show two samples, and there were significant differences
Table 5 early April dispensing district and the female mouse investigation in check plot
| Project | Contrast (12) | Handle (13) |
| Average weight (g) | 51.63±3.65 | 51.7±1.76 |
| Average carcass weight (g) | 35.93±2.03 | 38.81±1.38 |
| The vaginal opening number of |
10 | 13 |
| Vaginal opening rate (%) | 83.3 | 100 |
| Conceived number of elements | 7 | 10 |
| Pregnancy rate (%) | 58.33 | 76.92 |
| Average litter size | 5.57 | 4.4 |
| The stillborn foetus number of elements | 0 | 8 |
| Still birth rate (%) | 0 | 8/10=80% ★ |
★ Chi-square Test (Chi-square Test) shows two samples, and there were significant differences
At duration of test, do not observe the phenomenon of the pharmaceutical chemistry of searching for food such as domestic animal (ox, sheep), birds, lizard, but pharmaceutical chemistry was only promptly searched for food totally in 3 days by muroid.Observe wild birds such as skylark simultaneously and seek peck at seed between grass but the phenomenon of the pharmaceutical chemistry of not pecking at.
Above-mentioned experiment shows that the present invention has following advantage with respect to prior art;
(1) adds peanut oil, naked oats face and hay meal in the bait and increased the palatability of muroid and the degree of packing of particle.
(2) bait formula is simple, and raw material is common to be easy to get, and saves grain.
(3) bait is pressed into long column strip particle bait grain, effectively avoids eating by mistake of non-target animal, and got food residue pharmaceutical chemistry by muroid and be easy to decompose, have environmental safety.
(4) the former medicine in bait compacting back is in the dry carrier, and drug effect can keep (term of validity 3 years) for a long time.
(5) fully be blended in all particles of bait owing to medicine; Each mouthful that muroid is eaten into all contains the identical medicine of concentration; Thereby only more meet the rodent foraging habit attached to the wheat surface with its medicine of pharmaceutical chemistry of traditional wheat configuration, can guarantee that medicine can play one's part to the full.
(6) use safety effectively alleviates the contamination of medicine to dispensing person.
Claims (10)
1. a rodents sterilant pharmaceutical chemistry is made up of basic bait component, warning colouration and the former medicine of apholate;
Wherein, basic bait component is made up of following component:
Maize pulp or ground rice 10~30%;
Naked oats flour 10~30%;
Hay meal 55~60%;
Peanut oil 0.5~0.7%;
Said percentage composition is the quality percentage composition.
2. rodents sterilant pharmaceutical chemistry according to claim 1 is characterized in that: said basic bait component is following 1)-3) in any described component:
1) form by following component:
Maize pulp 29.5%;
Naked oats flour 10%;
Hay meal 60%;
Peanut oil 0.5%;
2) form by following component:
Maize pulp 10%;
Naked oats flour 29.3%;
Hay meal 60%;
Peanut oil 0.7%;
3) form by following component:
Ground rice 10%;
Naked oats flour 29.3%;
Hay meal 60%;
Peanut oil 0.7%;
Said percentage composition is the quality percentage composition.
3. rodents sterilant pharmaceutical chemistry according to claim 1 and 2 is characterized in that: said warning colouration is edible light blue, and its addition is 0.01% of a said basic bait constituent mass.
4. according to any described rodents sterilant pharmaceutical chemistry among the claim 1-3, it is characterized in that: the former medicine of apholate is that quinestrol and Levonorgestrel are mixing in 1: 2 according to weight ratio, and the addition of the former medicine of apholate is 0.005% of a said basic bait constituent mass.
5. according to any described rodents sterilant pharmaceutical chemistry among the claim 1-4, it is characterized in that: said hay meal is Powdered pasture powder.
6. rodents sterilant pharmaceutical chemistry according to claim 5 is characterized in that: said hay meal is Powdered daghestan sweet clover, sheep's hay or clover.
7. according to any described rodents sterilant pharmaceutical chemistry among the claim 1-6, it is characterized in that: said rodents sterilant pharmaceutical chemistry is rolling growth 8-15mm, the cylindrical particle of the about 2-3mm of diameter.
8. the preparation method of the said rodents sterilant pharmaceutical chemistry of claim 1 comprises the steps:
(1) the former medicine of apholate is mixed with peanut oil, container is placed 40-60 ℃ of water-bath 40min, and constantly stir and make it dissolving and obtain original liquid;
(2) the good original liquid of (1) dissolving is poured in the naked oats flour and is fully stirred soup is uniformly dispersed, during add warning colouration and stir, be made into female powder I;
(3) the female powder I that (2) is made into fully mixes with maize pulp or rice ground rice, stirs with agitator to make it to mix, and is made into female powder II;
(4) the female powder II that (3) is made into mixes with hay meal, stirs, and is made into the pharmaceutical chemistry powder;
(5) the pharmaceutical chemistry powder that (4) is made into mixes after the proper amount of clear water at the rolling growth 8~15mm of granule, and the cylindrical particle of the about 3mm of diameter, natural air drying obtain the rodents sterilant pharmaceutical chemistry;
The addition of above-mentioned each component adds according to the constituent content of embodiment 1.
9. method according to claim 8 is characterized in that: among the preparation method of said rodents sterilant pharmaceutical chemistry used each component with and addition add according to claim 2.
10. method according to claim 8 is characterized in that: among the preparation method of said rodents sterilant pharmaceutical chemistry used each component with and addition add according to claim 3 or claim 4.
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| CN2010102795471A CN102396476A (en) | 2010-09-10 | 2010-09-10 | Murine sterilant bait for controlling rodent damage in farmland and grassland |
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| CN2010102795471A CN102396476A (en) | 2010-09-10 | 2010-09-10 | Murine sterilant bait for controlling rodent damage in farmland and grassland |
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Cited By (1)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| CN103783052A (en) * | 2014-01-24 | 2014-05-14 | 河南科技大学 | Novel rodent sterile bait and preparation method thereof |
Citations (1)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| CN1500387A (en) * | 2002-11-13 | 2004-06-02 | 中国科学院动物研究所 | Bait for controlling the fertility number of rats and the use thereof |
-
2010
- 2010-09-10 CN CN2010102795471A patent/CN102396476A/en active Pending
Patent Citations (1)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| CN1500387A (en) * | 2002-11-13 | 2004-06-02 | 中国科学院动物研究所 | Bait for controlling the fertility number of rats and the use thereof |
Non-Patent Citations (3)
| Title |
|---|
| CHAMBERS LK 等: "Biological control of rodents-the case for fertility control using immunocontraception", 《ECOLOGICALLY-BASED RODENT MANAGEMENT》, no. 59, 31 December 1999 (1999-12-31), pages 215 - 242 * |
| 宛新荣 等: "EP-1不育剂对黑线毛足鼠种群繁殖的影响", 《兽类学报》, vol. 26, no. 4, 31 December 2006 (2006-12-31), pages 392 - 397 * |
| 霍秀芳 等: "左炔诺孕酮-炔雌醚对长爪沙鼠的不育效果", 《植物保护学报》, vol. 34, no. 3, 30 June 2007 (2007-06-30), pages 321 - 325 * |
Cited By (1)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| CN103783052A (en) * | 2014-01-24 | 2014-05-14 | 河南科技大学 | Novel rodent sterile bait and preparation method thereof |
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Application publication date: 20120404 |