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. 2022 Oct 19;27(20):7052. doi: 10.3390/molecules27207052

Table 1.

Summary of hormones and their effects on lipid production and decomposition.

Hormone Lipid Synthesis Lipid Catabolism
Insulin Promotion
SREBP-1C, ChREBP↑ [7,8,11]
FoxO1↓ [15]
Glucagon Inhibition
1. SREBP-1C, ChREBP↓ [28,29]
2. ACC↓ [28,29]
Promotion
1. PPARα, Aox, CTP1, Ctp1a↑ [28,29]
2. ACC↓ [28,29]
3. HSL in adipocytes↑ [34,39,40,41]
Thyroid
hormone
Promotion
1. SREBP-1C [56,57], ChREBP↑ [55]
2. ACC, Fasn↑ [65]
3. FATPs, L-FABPs↑ [60,61,62]
4. HMG-CoA Reductase↑ [75]
Inhibition
5. PPARγ↓ [51]
Promotion
1. HSL [69,70,71], ATGL↑ [70,71]
2. PPARα↑ [53]
3. Lipophagy↑ [80]
4. PGC1α, mtTFA↑ [82]
5. MCAD [86], PDK4 [87], UCP2↑ [88]
6. CYP7A1↑ [76]
Estrogen Inhibition
1. PPARγ↓ [110]
2. ACC, Fasn↓ [110]
Progesterone Promotion
1. SREBP↑ [113]
Androgen Promotion
1. SREBP, ChREBP↑ [116,117]
2. ACC, Fasn↑ [115]
Promotion
[119,120]
Growth
homone
Inhibition
1. PPARγ↓ [164,165,166]
2. Reducing insulin sensitivity [158]
Promotion
1. WAT lipolysis↑ [156]
2. HSL↑ [160,161,162]

SREBP, ChREBP and FoxO are important transcription factor regulating lipid production. PPARα promotes FFA β-oxidation by stimulating the transcription of FFA β-oxidation genes such as Aox, Ctp1a. PPARγ plays a role in promoting lipid synthesis. HSL and ATGL are enzymes that catalyze lipolysis. MCAD, PDK4, UCP2 are important enzymes in β-oxidation. FATPs and L-FABPs are protein transporters which mediate FFA-entering hepatocytes for substrates of liver TG synthesis.