Physiology and biochemistry of Drosophila learning mutants

被引:251
作者
Davis, RL [1 ]
机构
[1] BAYLOR COLL MED, DEPT NEUROL, HOUSTON, TX 77030 USA
关键词
D O I
10.1152/physrev.1996.76.2.299
中图分类号
Q4 [生理学];
学科分类号
071003 ;
摘要
Single gene mutants of Drosophila that are defective in learning/memory processes have increased substantially our understanding of the physiology, biochemistry, and anatomy underlying conditioned behaviors. Drosophila learning mutants can be separated into two general classes, those with structural defects in the brain and those without (conditioning mutants) any obvious brain alterations. From studies of brain structural mutants, two neuroanatomic areas have merged as important for normal conditioned behavior: the mushroom bodies and the central complex. Biochemical and molecular genetic studies of the conditioning mutants have implicated numerous types of molecules in learning, but the adenosine 3',5'-cyclic monophosphate (cAMP) second messenger pathway has emerged as especially important. Five different genes in this pathway, amnesiac (a product similar to adenylate cyclase activating peptides), dunce (cAMP phosphodiesterase), rutabaga (adenylyl cyclase), DCO (protein kinase A), and dCREB2 (cAMP-response element binding protein), have proven important for normal learning. The products of many of these learning mutants are enriched in mushroom bodies, which highlight the importance of mushroom bodies for normal learning and the cAMP second messenger cascade for the physiology of mushroom body cells in their role(s) underlying learning. Physiological studies of the mutants have demonstrated that plastic propel-ties of synaptic transmission, including facilitation and posttetanic potentiation, are abnormal in the mutants. An appendix describing the currently used paradigms to test Drosophila behavior is included.
引用
收藏
页码:299 / 317
页数:19
相关论文
共 98 条
[41]  
FUSTER JM, 1982, J NEUROSCI, V2, P361
[42]  
GAILEY DA, 1982, GENETICS, V102, P771
[43]   CYCLIC-AMP STIMULATES SOMATOSTATIN GENE-TRANSCRIPTION BY PHOSPHORYLATION OF CREB AT SERINE-133 [J].
GONZALEZ, GA ;
MONTMINY, MR .
CELL, 1989, 59 (04) :675-680
[44]   INHIBITION OF CALCIUM CALMODULIN-DEPENDENT PROTEIN-KINASE IN DROSOPHILA DISRUPTS BEHAVIORAL PLASTICITY [J].
GRIFFITH, LC ;
VERSELIS, LM ;
AITKEN, KM ;
KYRIACOU, CP ;
DANHO, W ;
GREENSPAN, RJ .
NEURON, 1993, 10 (03) :501-509
[45]   CALCIUM/CALMODULIN-DEPENDENT PROTEIN-KINASE-II AND POTASSIUM CHANNEL SUBUNIT EAG SIMILARLY AFFECT PLASTICITY IN DROSOPHILA [J].
GRIFFITH, LC ;
WANG, J ;
ZHONG, Y ;
WU, CF ;
GREENSPAN, RJ .
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1994, 91 (21) :10044-10048
[46]   PREFERENTIAL EXPRESSION OF THE DROSOPHILA RUTABAGA GENE IN MUSHROOM BODIES, NEURAL CENTERS FOR LEARNING IN INSECTS [J].
HAN, PL ;
LEVIN, LR ;
REED, RR ;
DAVIS, RL .
NEURON, 1992, 9 (04) :619-627
[47]  
Heisenberg M., 1989, Progress in Zoology, V37, P3
[48]   STRUCTURAL PLASTICITY IN THE DROSOPHILA BRAIN [J].
HEISENBERG, M ;
HEUSIPP, M ;
WANKE, C .
JOURNAL OF NEUROSCIENCE, 1995, 15 (03) :1951-1960
[49]   DROSOPHILA MUSHROOM BODY MUTANTS ARE DEFICIENT IN OLFACTORY LEARNING [J].
HEISENBERG, M ;
BORST, A ;
WAGNER, S ;
BYERS, D .
JOURNAL OF NEUROGENETICS, 1985, 2 (01) :1-30
[50]  
JELLIES JA, 1981, THESIS ILLINOIS STAT