top
Please input keywords
Order
*Country
United States
China
France
Germany
Netherlands
United Kingdom
Japan
South Korea
Israel
Australia
Hong Kong, China
New Zealand
Russia
Singapore
Taiwan, China
India
Aland Islands
Albania
Algeria
American Samoa
Andorra
Angola
Anguilla
Antarctica
Antigua & Barbuda
Argentina
Armenia
Aruba
Ascension Island
Austria
Azerbaijan
Bahamas
Bahrain
Bangladesh
Barbados
Belarus
Belgium
Belize
Benin
Bermuda
Bhutan
Bolivia
Bosnia & Herzegovina
Botswana
Brazil
British Indian Ocean Territory
British Virgin Islands
Brunei
Bulgaria
Burkina Faso
Burundi
Cambodia
Cameroon
Canada
Canary Islands
Cape Verde
Caribbean Netherlands
Cayman Islands
Central African Republic
Ceuta & Melilla
Chad
Chile
Christmas Island
Cocos (Keeling) Islands
Colombia
Comoros
Congo - Brazzaville
Congo - Kinshasa
Cook Islands
Costa Rica
Côte d’Ivoire
Croatia
Cuba
Curaçao
Cyprus
Czechia
Denmark
Diego Garcia
Djibouti
Dominica
Dominican Republic
Ecuador
Egypt
El Salvador
Equatorial Guinea
Eritrea
Estonia
Ethiopia
Falkland Islands
Faroe Islands
Fiji
Finland
French Guiana
French Polynesia
French Southern Territories
Gabon
Gambia
Georgia
Ghana
Gibraltar
Greece
Greenland
Grenada
Guadeloupe
Guam
Guatemala
Guernsey
Guinea
Guinea-Bissau
Guyana
Haiti
Honduras
Hungary
Iceland
Indonesia
Iran
Iraq
Ireland
Isle of Man
Italy
Jamaica
Jersey
Jordan
Kazakhstan
Kenya
Kiribati
Kosovo
Kuwait
Kyrgyzstan
Laos
Latvia
Lebanon
Lesotho
Liberia
Libya
Liechtenstein
Lithuania
Luxembourg
Macau, China
Macedonia
Madagascar
Malawi
Malaysia
Maldives
Mali
Malta
Marshall Islands
Martinique
Mauritania
Mauritius
Mayotte
Mexico
Micronesia
Moldova
Monaco
Mongolia
Montenegro
Montserrat
Morocco
Mozambique
Myanmar (Burma)
Namibia
Nauru
Nepal
New Caledonia
Nicaragua
Niger
Nigeria
Niue
Norfolk Island
North Korea
Northern Mariana Islands
Norway
Oman
Pakistan
Palau
Palestinian Territories
Panama
Papua New Guinea
Paraguay
Peru
Philippines
Pitcairn Islands
Poland
Portugal
Puerto Rico
Qatar
Réunion
Romania
Rwanda
Samoa
San Marino
São Tomé & Príncipe
Saudi Arabia
Senegal
Serbia
Seychelles
Sierra Leone
Sint Maarten
Slovakia
Slovenia
Solomon Islands
Somalia
South Africa
South Georgia & South Sandwich Islands
South Sudan
Spain
Sri Lanka
St. Barthélemy
St. Helena
St. Kitts & Nevis
St. Lucia
St. Martin
St. Pierre & Miquelon
St. Vincent & Grenadines
Sudan
Suriname
Svalbard & Jan Mayen
Swaziland
Sweden
Switzerland
Syria
Tajikistan
Tanzania
Thailand
Timor-Leste
Togo
Tokelau
Tonga
Trinidad & Tobago
Tristan da Cunha
Tunisia
Turkey
Turkmenistan
Turks & Caicos Islands
Tuvalu
U.S. Outlying Islands
U.S. Virgin Islands
Uganda
Ukraine
United Arab Emirates
United Nations
Uruguay
Uzbekistan
Vanuatu
Vatican City
Venezuela
Vietnam
Wallis & Futuna
Western Sahara
Yemen
Zambia
Zimbabwe
*Province
*City
*Name
*Telephone
*Company
*Position
*Email
*Verification code
*Verification Code
B-hCB1 mice
Strain Name
C57BL/6-Cnr1tm1(CNR1)Bcgen/Bcgen 
Common Name  B-hCB1 mice
Background C57BL/6N Catalog number  110943
Related Genes 
CANN6, CB-R, CB1, CB1A, CB1K5, CB1R, CNR
NCBI Gene ID
12801

mRNA expression analysis


from clipboard


Strain specific analysis of CB1 gene expression in wild-type C57BL/6 mice and B-hCB1 mice by RT-PCR. Mouse CB1 mRNA was detectable only in cerebellum and brain cells of wild-type C57BL/6 mice (+/+). Human CB1 mRNA was detectable only in cerebellum and brain cells of homozygous B-hCB1 mice (H/H), but not in wild-type mice. 

Protein expression analysis

from clipboard


Strain specific CB1 expression analysis in homozygous B-hCB1 mice by western blot. Cerebellum and brain tissue was collected from wild-type C57BL/6 mice (+/+) and homozygous B-hCB1 mice (H/H) and analyzed by western blot with anti-CB1 antibody which was cross reactive between mouse and human. Mouse and human CB1 were detectable in wild-type mice and homozygous B-hCB1 mice. 

In vivo efficacy of DIO model in B-hCB1 mice

from clipboard


Weight of DIO model in B-hCB1 mice. 30 homozygous animals were randomly divided into 2 groups according to their body weight, 8 animals in group A, fed with STD and 22 animals in Group B, fed with HFD. DIO model of B-hCB1 mice was induced by HFD for 12 weeks, then randomly divided into 3 groups(G2, G3, and G4) and treated with vehicle, antagonists, and dulaglutide respectively(n=7-8). (A) The schematic diagram of experimental processing. (B) Body weight after 12 weeks of DIO. (C-D) Body weight and weight changes in each group after treatment. As shown in Figure B, compared with the group STD, the weight of the HFD group were significantly increased, indicating that B-hCB1 mice can successfully induce obesity models. As shown in Figure C and D, compared with the HFD vehicle group, CB1 antagonists and dulaglutide can significantly reduce the weight. Values are expressed as mean ± SEM.

from clipboard


CB1 antagonist reduces blood glucose in male B-hCB1 mice. (A) Random blood glucose. (B) Fasting blood glucose in Day 27 post treatment. (C-D) Glucose tolerance test. As shown in the figure, the CB1 antagonist and dulaglutide can reduce the random blood glucose and fasting blood glucose and improve glucose tolerance in male B-hCB1 mice. Values are expressed as mean ± SEM.

from clipboard


CB1 antagonist improved lipid metabolism in male B-hCB1 mice. (A) TG in liver. (B) TC in liver. (C) TG in blood. (D) TG in blood. As shown in the figure, the CB1 antagonist and dulaglutide can reduce the level of TG in liver and TC in blood. Values are expressed as mean ± SEM.

from clipboard


CB1 antagonist reduced liver damage caused by diet induced obesity in male B-hCB1 mice. (A) Representative H&E-stained liver images (representative dataset from n = 7-8 per group). (B) Statistical analysis of scores for hepatocellular steatosis, lobular inflammation and ballooning degeneration of liver cells. Values are expressed as mean ± SD. *p<0.05.