Diet-induced obese mice develop peripheral, but not central, resistance to leptin

被引：643

作者：

VanHeek, M ^{[1
]}

Compton, DS ^{[1
]}

France, CF ^{[1
]}

Tedesco, RP ^{[1
]}

Fawzi, AB ^{[1
]}

Graziano, MP ^{[1
]}

Sybertz, EJ ^{[1
]}

Strader, CD ^{[1
]}

Davis, HR ^{[1
]}

机构：

[1] SCHERING PLOUGH CORP,RES INST,CARDIOVASC RES,KENILWORTH,NJ 07033

来源：

JOURNAL OF CLINICAL INVESTIGATION | 1997年 / 99卷 / 03期

关键词：

leptin resistance; high fat diet; food intake; C57BL/6; AKR;

D O I：

10.1172/JCI119171

中图分类号：

R-3 [医学研究方法]; R3 [基础医学];

学科分类号：

1001 ;

摘要：

Leptin administration reduces obesity in leptin-deficient ob/ob mice; its effects in obese humans, who have high circulating leptin levels, remain to be determined. This longitudinal study was designed to determine whether diet-induced obesity in mice produces resistance to peripheral and/or central leptin treatment. Obesity was induced in two strains of mice by exposure to a 45% fat diet. Serum leptin increased in proportion to body weight (P <0.00001). Whereas C57BL/6 mice initially responded to peripherally administered leptin with a marked decrease in food intake, leptin resistance developed after 16 d on high fat diet; mice on 10% fat diet retained leptin sensitivity. In AKR mice, peripheral leptin significantly decreased food intake in both 10 and 45% fat-fed mice after 16 d of dietary treatment. However, after 56 d, both groups became resistant to peripherally administered leptin. Central administration of leptin to peripherally leptin-resistant AKR mice on 45% fat diet resulted in a robust response to leptin, with a dose-dependent decrease in food intake (P <0.00001) and body weight (P <0.0001) after a single intracerebroventricular infusion. These data demonstrate that, in a diet-induced obesity model, mice exhibit resistance to peripherally administered leptin, while retaining sensitivity to centrally administered leptin.

引用

页码：385 / 390

页数：6

共 25 条

[1] Expression and purification of a synthetic human obese gene product
Altmann, SW
Timans, JC
Rock, FL
Bazan, JF
Kastelein, RA
[J]. PROTEIN EXPRESSION AND PURIFICATION, 1995, 6 (06) : 722 - 726
[2] Leptin enters the brain by a saturable system independent of insulin
Banks, WA
Kastin, AJ
Huang, WT
Jaspan, JB
Maness, LM
[J]. PEPTIDES, 1996, 17 (02) : 305 - 311
[3] RECOMBINANT MOUSE OB PROTEIN - EVIDENCE FOR A PERIPHERAL SIGNAL LINKING ADIPOSITY AND CENTRAL NEURAL NETWORKS
CAMPFIELD, LA
SMITH, FJ
GUISEZ, Y
DEVOS, R
BURN, P
[J]. SCIENCE, 1995, 269 (5223) : 546 - 549
[4] Decreased cerebrospinal-fluid/serum leptin ratio in obesity: A possible mechanism for leptin resistance
Caro, JF
Kolaczynski, JW
Nyce, MR
Ohannesian, JP
Opentanova, I
Goldman, WH
Lynn, RB
Zhang, PL
Sinha, MK
Considine, RV
[J]. LANCET, 1996, 348 (9021) : 159 - 161
[5] EVIDENCE AGAINST EITHER A PREMATURE STOP CODON OR THE ABSENCE OF OBESE GENE MESSENGER-RNA IN HUMAN OBESITY
CONSIDINE, RV
CONSIDINE, EL
WILLIAMS, CJ
NYCE, MR
MAGOSIN, SA
BAUER, TL
ROSATO, EL
COLBERG, J
CARO, JF
[J]. JOURNAL OF CLINICAL INVESTIGATION, 1995, 95 (06) : 2986 - 2988
[6] CONSIDINE RV, 1996, DIABETES, V19, P992
[7] EXPRESSION OF OB MESSENGER-RNA AND ITS ENCODED PROTEIN IN RODENTS - IMPACT OF NUTRITION AND OBESITY
FREDERICH, RC
LOLLMANN, B
HAMANN, A
NAPOLITANOROSEN, A
KAHN, BB
LOWELL, BB
FLIER, JS
[J]. JOURNAL OF CLINICAL INVESTIGATION, 1995, 96 (03) : 1658 - 1663
[8] LEPTIN LEVELS REFLECT BODY LIPID-CONTENT IN MICE - EVIDENCE FOR DIET-INDUCED RESISTANCE TO LEPTIN ACTION
FREDERICH, RC
HAMANN, A
ANDERSON, S
LOLLMANN, B
LOWELL, BB
FLIER, JS
[J]. NATURE MEDICINE, 1995, 1 (12) : 1311 - 1314
[9] RATIONAL DESIGN OF POTENT ANTAGONISTS TO THE HUMAN GROWTH-HORMONE RECEPTOR
FUH, G
CUNNINGHAM, BC
FUKUNAGA, R
NAGATA, S
GOEDDEL, DV
WELLS, JA
[J]. SCIENCE, 1992, 256 (5064) : 1677 - 1680
[10] WEIGHT-REDUCING EFFECTS OF THE PLASMA-PROTEIN ENCODED BY THE OBESE GENE
HALAAS, JL
GAJIWALA, KS
MAFFEI, M
COHEN, SL
CHAIT, BT
RABINOWITZ, D
LALLONE, RL
BURLEY, SK
FRIEDMAN, JM
[J]. SCIENCE, 1995, 269 (5223) : 543 - 546

← 1 2 3 →