Autophagy is a self-degradation process that is important to sustain cell homeostasis responding to nutrient stresses and extracellular signals. During autophagy, a part of cytoplasm is engulfed by double-membrane autophagosomes, which fuse with the vacuole for degradation. Many protein complexes are involved. Several researches have proved that membrane trafficking pathway is involved in autophagy regulation. The Ypt/Rab GTPase protein family is one of the important protein complex regulating membrane trafficking. Previous studies have shown that Ypt1 and Ypt7 could both regulate autophagy process. Ypt1 regulates the formation of Atg1/Atg13 complex, a requirement of autophagy induction. On the other hand, Ypt7 is the essential factor for fusion between autophagosomes and the vacuole. Activity of Ypt/Rab GTPase proteins are modulated by guanine-nucleotide exchange factors (GEFs) and GTPase activation proteins (GAPs). Gyp1 is the GAP protein of Ypt1 and Ypt7 in yeast. In my study, gyp1D cells showed bulk autophagy and Cvt pathway defect. gyp1D cells also had conventional membrane trafficking defect phenotype.