444 results on '"Lorenzi, Cristina"'
Search Results
102. Catechol-O-methyltransferase gene variants in mood disorders in the Italian population
103. Serotonin transporter gene-linked polymorphic region: possible pharmacogenetic implications of rare variants
104. Lack of genetic association between the phospholipase A2 gene and bipolar mood disorder in a European multicentre case–control study
105. Analysis of COMT gene (Val 158 Met polymorphism) in the clinical response to SSRIs in depressive patients of European origin
106. Temperament and Character in Mood Disorders: Influence of DRD4, SERTPR, TPH and MAO-A Polymorphisms
107. Further evidence of MAO-A gene variants associated with bipolar disorder
108. 5-HT1A polymorphism and self-transcendence in mood disorders
109. Two new rare variants in the circadian “clock” gene may influence sleep pattern
110. Social adjustment could be associated with the serotonin transporter gene in remitted patients with mood disorders and healthy subjects
111. Long-term response to lithium salts in bipolar illness is influenced by the glycogen synthase kinase 3-β −50 T/C SNP
112. Interaction between the Tryptophan Hydroxylase Gene and the Serotonin Transporter Gene in Schizophrenia but Not in Bipolar or Unipolar Affective Disorders
113. The C(–1019)G polymorphism of the 5-HT1A gene promoter and antidepressant response in mood disorders: preliminary findings
114. Tardive dyskinesia and DRD2, DRD3, DRD4, 5-HT2A variants in schizophrenia: an association study with repeated assessment
115. Genetic dissection of drug effects in clinical practice: CLOCK gene and clozapine-induced diurnal sleepiness
116. A glycogen synthase kinase 3-β promoter gene single nucleotide polymorphism is associated with age at onset and response to total sleep deprivation in bipolar depression
117. The Use of DNA Microarray in the Pharmacogenetics of Antidepressants: Guidelines for a Targeted Approach
118. New Antipsychotics and Schizophrenia: A Review on Efficacy and Side Effects
119. A single nucleotide polymorphism in glycogen synthase kinase 3-β promoter gene influences onset of illness in patients affected by bipolar disorder
120. Influence ofCLOCK gene polymorphism on circadian mood fluctuation and illness recurrence in bipolar depression
121. Multicentre Italian family-based association study on tyrosine hydroxylase, catechol-O-methyl transferase and Wolfram syndrome 1 polymorphisms in mood disorders
122. Genetic dissection of psychopathological symptoms: Insomnia in mood disorders and CLOCK gene polymorphism
123. Association study of MAO‐A, COMT, 5‐HT2A, DRD2, and DRD4 polymorphisms with illness time course in mood disorders
124. Family-based association study of 5-HTTLPR, TPH, MAO-A, and DRD4 polymorphisms in mood disorders
125. Pharmacogenetics of lithium prophylaxis in mood disorders: Analysis of COMT, MAO-A, and G?3 variants
126. Influence of monoamine oxidase A and serotonin receptor 2A polymorphisms in SSRI antidepressant activity
127. No association between dopamine D2 and D4 receptor gene variants and antidepressant activity of two selective serotonin reuptake inhibitors
128. DRD4 exon 3 variants associated with delusional symptomatology in major psychoses: A study on 2,011 affected subjects
129. Serotonin-2C and serotonin-1A receptor genes are not associated with psychotic symptomatology of mood disorders
130. Serotonin-2A receptor gene is not associated with symptomatology of schizophrenia
131. No interaction between serotonin transporter gene and dopamine receptorD4 gene in symptomatology of major psychoses
132. No interaction between serotonin transporter gene and dopamine receptor D4 gene in symptomatology of major psychoses
133. Dopamine D3 receptor gene not associated with symptomatology of major psychoses
134. Dopamine receptor D2 and D4 genes, GABAA alpha-1 subunit gene and response to lithium prophylaxis in mood disorders
135. Dopamine receptor D3 gene and response to lithium prophylaxis in mood disorders
136. Lithium and GSK3-β Promoter Gene Variants Influence White Matter Microstructure in Bipolar Disorder.
137. Searching Susceptibility Loci for Bipolar Disorder: A Sib Pair Study on Chromosome 12.
138. DRD4 exon 3 variants are not associated with symptomatology of major psychoses in a German population
139. Further evidence of MAO‐A gene variants associated with bipolar disorderPlease cite this article as follows: Müller DJ, Serretti A, Sicard T, Tharmalingam S, King N, Artioli P, Mandelli L, Lorenzi C, Kennedy JL. 2007. Further Evidence of MAO‐A Gene Variants Associated With Bipolar Disorder. Am J Med Genet Part B 144B:37–40.
140. Genetic dissection of psychopathological symptoms: Insomnia in mood disorders and <TOGGLE>CLOCK</TOGGLE> gene polymorphism
141. Multicentre Italian familybased association study on tyrosine hydroxylase, catecholOmethyl transferase and Wolfram syndrome 1 polymorphisms in mood disorders
142. No interaction between serotonin transporter gene and dopamine receptor <TOGGLE>D4</TOGGLE> gene in symptomatology of major psychoses
143. Multimodal brain-derived subtypes of Major depressive disorder differentiate patients for anergic symptoms, immune-inflammatory markers, history of childhood trauma and treatment-resistance.
144. Selective association of cytokine levels and kynurenine/tryptophan ratio with alterations in white matter microstructure in bipolar but not in unipolar depression.
145. Internal Synchrony and Mood: A Study of Circadian Misalignment in Bipolar Depression
146. Low-dose interleukin 2 antidepressant potentiation in unipolar and bipolar depression: Safety, efficacy, and immunological biomarkers.
147. Choroid plexus volume is increased in mood disorders and associates with circulating inflammatory cytokines.
148. Circulating cytotoxic immune cell composition, activation status and toxins expression associate with white matter microstructure in bipolar disorder.
149. Melatonin secretion patterns are associated with cognitive vulnerability and brain structure in bipolar depression.
150. Insulin resistance disrupts white matter microstructure and amplitude of functional spontaneous activity in bipolar disorder.
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