1. Introduction
Intracellular redox balance is crucial for neurophysiology and might be a trigger in the pathogenesis of mental diseases [
1,
2]. Undoubtedly, antioxidants are vital for maintaining brain homeostasis. Oxidative stress and its dysregulation play a significant role in the pathophysiology of schizophrenia (SZ) in endothelial dysfunction and atherosclerosis development [
3]. Lower levels of paraoxonase 1 (PON-1) and peroxidase glutathione (GPx) are associated with abnormal expression of pro-inflammatory genes and their products, such as interleukins and cell adhesion molecules. Additionally, this decrease in antioxidant enzyme activity contributes to a reduction in anti-oxidative activity [
4]. Intracellular adhesion molecule (ICAM), vascular cell adhesion molecules (VCAM), and monocyte chemoattractant protein-1 (MCP-1) promotes the infiltration of monocytes to the vascular wall and leads to an increase in local, causing endothelial dysfunction consequently—a key point of atherosclerotic plaque genesis [
5,
6].
There are still areas that are insufficiently explored and attract the attention of researchers. One such area pertains to the molecular mechanisms underlying the development of dyslipidemia in peripheral blood vessels and its impact on brain function and lipid levels within the central nervous system (CNS) during acute psychotic decompensation in individuals diagnosed with SZ. Based on the literature, the blood–brain barrier (BBB) is impermeable to lipids, and cholesterol is synthesized de novo in the CNS [
7,
8]. Furthermore, the brain contains about 20% of the whole body’s cholesterol and is the most cholesterol-rich organ [
8]. Nevertheless, only high-density lipoproteins (HDL) have the capability to cross the blood–brain barrier (BBB) through a process called transcytosis [
9]. This process involves HDL interacting with the scavenger receptor BI (SR-BI) present in the brain’s capillary endothelial cells [
10]. SR-BI is known for its crucial role in HDL metabolism in the liver, but it is also present in the brain, facilitating the transport of HDL across the BBB. Low peripheral HDL levels may intensify inflammatory processes, increase the severity of atherosclerotic lesions in cerebral blood vessels [
11,
12] and influence the function of the endothelium in cerebral vessels, consequently affecting neuronal function. Cholesterol is crucial for various neuronal processes, including membrane integrity, synaptic function, and neurotransmitter receptor signaling. HDL helps regulate the distribution and transport of cholesterol within the CNS, ensuring a balance and proper availability of cholesterol for neuronal function [
7]. In the context of SZ pathogenesis, multiple studies have explored the correlation between lipid profiles and the CNS physiology. Dyslipidemia, including alterations in HDL levels, has been associated with abnormalities in brain structure and function observed in SZ. Abnormal lipid metabolism and disturbances in cholesterol homeostasis may contribute to neurodevelopmental abnormalities, synaptic dysfunction, and impaired neurotransmission implicated in SZ.
Schizophrenia is a widespread chronic mental disorder, affecting about 1% of the world population [
1], or up to 20 million people around the world [
2]. Unfortunately, this complex disease with unknown etiology is still an actual medical and social problem in plenty of countries. Patients suffering from SZ no doubt have a poor prognosis, accompanied by a risk of somatic disorders and worsening psychiatric functioning. The primary identification of SZ is mostly based on common signs of psychopathological status, as well as behavioral and clinical symptoms [
13,
14]. The average age of SZ onset in men is 18–25, while in women it is between 25 and 35 years of age. The prodromal phase can be observed even up to 30 months before onset [
13,
15]. The life span of patients diagnosed with schizophrenia is 20 years shorter than the average of the general population [
16]. During the last few decades, despite significant progress in medicine, the life span has not been elongated, but even become shorter. This observation is usually understood as a result of patients’ lifestyle, suicides, negative effects of pharmacotherapy, or limited access to treatment of somatic complications due to disease and socioeconomic status. The main risk factors in this regard are those associated with cardiometabolic complications. The most important in this context is the interaction between lipid metabolism disorders, oxidative balance disorders, and changes in peripheral vessels [
2,
17].
Schizophrenia is a complex mental disorder characterized by a wide range of symptoms. These symptoms are typically categorized into two groups: positive symptoms and negative symptoms. Positive symptoms are disturbances that are not typically present in healthy individuals (hallucinations, delirium, disorganized behavior), while negative symptoms involve the absence or reduction of normal behaviors and functions (anhedonia, a lack of movement, flat affect). The symptoms of SZ can be assessed using the Positive and Negative Syndrome Scale (PANSS) or the Brief Negative Symptoms Scale (BNSS) [
2,
18,
19]. It is also unclear to what extent other mental disorders such as bipolar disorder, obsessive-compulsive disorder, or some of somatic disorders have a constellation of risk factors like SZ. For instance, the common feature in the pathogenesis of SZ and bipolar disorder might be immune activation. Subtle disorganization of thought processes and impairment of cognitive functions such as memory, attention, or learning may precede the appearance of a full-blown clinical syndrome by many months, if not years [
1,
13]. Uncertain etiology, a pallet of symptoms, and an inevitability of prognosis reflect difficulties of studying, emphasizing its necessity.
One of the important doubts appearing in the literature is to what extent schizophrenia is a disorder of the brain itself, manifested in the psychosocial functioning of the patient, and to what extent it is a systemic disorder in which pathophysiological phenomena concern not only the central nervous system but also the periphery. In recent years, the lipid profile, endothelial function, and role of oxidative stress have been widely discussed in the literature in the context of SZ pathogenesis as well as its spectrum disorders [
12,
18,
20]. Metabolic disturbances are common in SZ. The lipid imbalance in such patients can be discussed in two different categories, sometimes combined: as side symptoms of treatment (some drugs lead to metabolic syndrome development) and as risk factor, impacted by severity and prognosis. Moreover, lipids may have their own role in inflammation development in SZ due to their involvement in oxidative stress in cells. The patients with first-episode psychosis without medication have lower levels of total cholesterol, low-density lipoproteins (LDL), and high-density lipoproteins (HDL), while their level of triglycerides is rising in comparison to healthy people. These changes were not related to age, gender, and body mass index (BMI) [
21]. Patients with SZ have also altered antioxidant functions [
22]. The interplay between lipid imbalance, oxidative stress, and inflammation may contribute to the increased vulnerability of individuals with SZ to cardiovascular complications.
Moreover, the first episode of SZ correlates with reductions in the essential omega-3 and omega-6 series of polyunsaturated fatty acids (PUFA) in erythrocytes membranes [
20]. The same tendency was common for the pathogenesis of bipolar disorder [
23]. The patients with first-episode psychosis demonstrated a declining in total oxidative resistance [
24]. The role of oxidative stress in psychiatric diseases (anxiety, depression, schizophrenia, autism) has been observed, using animal models and deep analysis of brain metabolism [
25,
26].
Brain morphology and physiology make a neurobiological basis for genesis of psychiatric diseases. A comprehensive understanding of the intricate pathophysiological processes in brain disorders allows us to clearly identify key points in the genesis of schizophrenia. Thus, we have focused our attention on several main biochemical parameters reflects in brain physiology. The frontal cortex, temporal pole, dorsal anterior cingulate cortex (ACC), and putamen are involved in pathogenesis of SZ [
27]. Lahutsina et al. suggested that the ACC gray matter reductions may presage psychosis onset [
28]. Another study focused on the role of redox imbalance/mitochondrial dysfunction and implicate interneuron subtypes in ACC in SZ pathophysiology [
29]. To note, patients with SZ have brains with a low pH (lower than normal) [
30]. Probably, structural and biochemical changes in particular areas of the human brain may lead to oxidative imbalance and disturbances in dopaminergic and glutamatergic transmissions as consequences. The glutamatergic theory of psychosis has been described by our scientific group previously [
31].
One of the most crucial parameters of lipid profile, which should be considered in analyses of risk factors and side effects in SZ, is HDL. Changes in HDL levels, whether declining or rising, may hold significance. As previously mentioned, decreased HDL levels have been observed in first-episode psychosis and SZ. Apolipoprotein A1 (ApoA1), as a component of HDL, and the antioxidative enzyme paraoxonase 1 (PON1), have anti-inflammatory, anti-atherogenic, antioxidant, and immunomodulatory roles. They are involved in the microenvironment in inflammations in the human body. Chronic SZ is characterized by an elevation of pro-inflammatory cytokines (interleukins (IL)-2, -6 and -10) [
32,
33,
34,
35].
Thus, inflammation may serve as a mechanism underlying the altered metabolism of lipids and, in conjunction with dyslipidemia, contribute to prefrontal cortex dysfunction, hippocampal impairments, and ultimately, the progression of psychotic symptoms in schizophrenia. We have hypothesized that dysfunction in the anterior cingulate gyrus (or in the prefrontal cortex) could be associated with lipid metabolism disorders during the first psychotic episode (FEP). However, evidence linking hippocampal alterations and lipid metabolism remains relatively limited. The aim of our innovative study was to comprehensively study the correlation between peripheral HDL levels and brain lipoproteins, as assessed by MRI scans, as well as peripheral oxidative stress as measured by paraoxonase.
3. Discussion
Psychiatric disorders are often accompanied by comorbidities (metabolic syndrome and cardiovascular diseases). Psychiatric patients may have an oxidative misbalance, which amplifies the risk of developing co-existing pathologies. The family of detoxifying enzymes, paraoxonases, includes three forms, and the first one (PON-1) is the most examined, while their role is still debatable. It is calcium-dependent enzyme, and is mostly expressed in the liver and in the kidneys [
37,
38], which are found in high-density lipoproteins (HDL) and in the intestinal cells [
39]. PON-1 was studied in patients with anxiety disorders, bipolar disorders, major depressive disorders, obsessive compulsory disorders, a major depression, and schizophrenia. Our former studies revealed a positive correlation between PON-1 activity, HDL, and levels and the concentration of free triiodothyronine after drug treatment [
37]. Based on the current literature data during the first episode of schizophrenia PON-1 activity is declined and is normalized only after appropriate therapy [
38]. Maes et al. concluded that schizophrenia is associated with decreased levels of natural IgM and reduced PON-1 activity (antioxidative and anti-inflammatory) [
40]. We have also observed lower activity of PON-1 in patients with SZ, which positively correlates with HDL levels and negatively correlates with LDL levels.
We suppose that oxidative imbalance and disturbances of immune microenvironment leads to neurodegeneration and manifestation of SZ, respectively. PON-1 enzymatic activity is associated with an intensity of kidney filtration: lower in patients with chronic kidney disease and hemodialysis [
41]. In patients with hemodialysis elevation of CRP (C-reactive protein—the parameter of inflammatory process), it is correlated with PON-1 decline which reflects a risk of cardiovascular complications in these patients [
42]. Our results demonstrate that the lowest level of PON-1 was in patients with schizophrenia, while the control group had higher concentrations. We can hypothesize that a decrease in PON-1 is associated with primary immunological disturbances and lower reparative and regenerative abilities. In such a group of people, the onset of schizophrenia could be observed. Based on data, PON-1 can transfer to the membrane, can be involved in HDL-mediated cholesterol outflow, and participate in the pathogenesis of oxidative stress-related diseases (including cardiovascular syndrome, HIV, metabolic syndrome) [
39,
43,
44,
45,
46]. All known types of PON have different rations between gene expression and protein detecting, based on the type) of tissue and disease, but all of them modulate the inflammation and oxidative stress. PON-1 could be transported by HDL from blood circulation through the blood–brain barrier to the brain and the cerebrospinal fluid [
39,
47]. The reason for this transport is still not clear. However, brain-cholesterol homeostasis is crucial for neurodegeneration development. For instance, Alzheimer’s disease is associated with a damage of oligodendrocytes from one side, and compensatory intensified transport of PON-1 to oligodendrocytes to reduce the oxidative imbalance from another side [
48]. The local inflammatory process leads to oxidative stress, in which PON-1 transported via HLD is involved as a force balancing redox reactions. Pro-inflammatory cytokines and neuroinflammation should be considered in the pathogenesis of SZ [
36], in which patients have a thinner cerebral cortex compared to healthy people on average [
48]. No doubt, mitochondrial dysfunction plays a role in the neurodegeneration in patients with neurological and psychiatric diseases (epilepsy, schizophrenia, multiple sclerosis, Alzheimer’s disease, Parkinson’s disease, Huntington’s disease).
The results obtained in this study are consistent with the results of the meta-analysis, which show that previously untreated patients with a first episode of non-affective psychosis showed significantly lower serum total cholesterol, LDL, and HDL levels compared to healthy controls [
49]. Lipid levels are very important for membrane balance, which is essential for myelin integrity [
50] and synaptic transmission [
7]. Although peripheral blood cholesterol cannot cross the blood–brain barrier (BBB), evidence suggests that there is a leakage between central and peripheral lipid metabolism that may ultimately affect central cholesterol concentrations [
7,
51]. The possible mechanism of the altered lipid profile in schizophrenia may be due to overlapping genetic risk factors for schizophrenia and the LDL and HDL profile [
52]. Gjerde et al. stressed that increasing HDL level during antipsychotic therapy is associated with improvement in negative symptoms in first-episode psychosis [
53,
54,
55,
56]. Another study depicted that abnormal HDL level might be an early-onset event in drug-naïve first-episode psychosis of adolescents and young adults who are unlikely to have other cardiometabolic risks [
32]. The relation between negative syndromes of SZ and metabolic abnormalities was observed by Wójciak et al.: women have a significant positive correlation between negative symptoms and HDL level, while men do not [
33].
Confounding factors such as drugs and disease duration may be involved, which together pose a problem in identifying altered connectivity between peripheral and central lipid metabolism. Our findings may reveal pathological changes in schizophrenia. In addition, structural analysis of prefrontal cortex regions including subfields of the hippocampus revealed reduced volume in first-episode psychotic patients. This result is consistent with other reports that emphasize that smaller hippocampal volume is already evident in the early stages of the first psychotic episode [
57].
In the presented study, one of the most interesting findings is the significant association between changes in total cholesterol and HDL levels and functional connectivity in the prefrontal cortex, which is in close proximity to the hippocampus. This association explains the lower cholesterol levels observed in schizophrenia patients, which are linked to higher prefrontal-hippocampal and thalamic-hippocampal connectivity. Membrane lipids, including cholesterol, are believed to be essential in maintaining membrane stability and neuronal function. Previous studies have shown that the synthesis and catabolism of cholesterol in the brain proceed dynamically in neurons affected by glutamate-mediated excitotoxicity, especially in the hippocampus [
58]. These findings closely correspond to our own results, which indicate that changes in glutamatergic transmission in the anterior cingulate gyrus turned out to be crucial in differentiating patients with schizophrenia [
31].
Furthermore, the observed negative correlation between serum HDL and DWI in the left cingulate cortex may indicate a potential mechanism, which can be explained by the fact that the lowered HDL cholesterol level is associated with increased functional connectivity in the prefrontal cortex in patients with schizophrenia. To the best of our knowledge, this study is the first to investigate the association between anterior cingulate disorder and high-density cholesterol levels in individuals with schizophrenia. Both in vitro and in vivo studies have shown that long-term exposure to excitatory neurotransmission can cause loss of membrane cholesterol in prefrontal cortex neurons [
58]. For instance, the study found a loss of up to 34% of cholesterol after 7 days of monosodium L-glutamate injection in the hippocampus of adult rats [
59]. The results indicate that treatment with high doses of NMDA agonists can then result in the lowering of cholesterol in hippocampal synaptosomes and loss of membrane cholesterol, accompanied by the upregulation and translocation of cholesterol-24-hydroxylase (Cyp46A1) to the surface of neurons; consequently, the site of the transition of cholesterol I to 24S-hydroxycholesterol and removes cholesterol from neurons. In such a situation, accelerated cholesterol loss may result in degeneration of the neural membrane, myelin, and axons of sensitive areas of the brain, indicating the disrupted integrity of the thalamic-hippocampal junctions also seen in our study. Astrocytes and microglia, both types of glial cells are essential for the nervous system, and insufficiency leads to neurodegeneration. Pathophysiology of SZ includes abnormalities in glial cells, especially astrocytes [
60]. Notter concluded that they can impact neurodevelopmental and homeostatic processes, connected with SZ pathogenesis [
61].
Other environmental factors, such as poor eating habits characterized by the consumption of high-calorie foods or saturated fatty acids, have been implicated in the development of neural imbalances and may contribute to the risk of schizophrenia. It is hypothesized that these dietary factors can disrupt the delicate balance of cholesterol in the brain, leading to dysfunction in critical brain regions involved in schizophrenia pathology. Specifically, the association between lowered serum cholesterol levels and dysfunction in the thalamic-hippocampal junction suggests a dynamic interplay between neuronal excitotoxicity responses and altered cholesterol balance during the early stages of schizophrenia.
According to our hypothesis, dysfunction in the anterior cingulate gyrus (or in the prefrontal cortex) is associated with lipid metabolism disorders during the psychotic episode. Among all metabolic markers, we observed significant intergroup differences in serum total and HDL cholesterol levels. There are few studies indicating the occurrence of subclinical dyslipidemia associated with low total cholesterol levels observed in patients with a first psychotic episode. This supports the hypothesis that lower cholesterol levels may be phenotypically important for people with previously untreated psychotic disorders. Similar observations were made in previously untreated patients prior to psychosis who had lower levels of total cholesterol, cholesterol esters, and phospholipids in the plasma membranes of skin fibroblasts [
62].
Our results are consistent with a meta-analysis in which previously untreated patients with a first episode of psychosis had significantly lower serum total cholesterol and HDL compared to healthy controls [
49]. Lipid levels are crucial for maintaining the balance of lipid membranes, which are an integral part of myelin [
50]. The possible mechanism of the altered lipid profile in schizophrenia may be due to the overlapping risk factors for schizophrenia, the broad spectrum of disease, and redox levels including HDL and PON-1 [
63].
Patients with SZ exhibit distinct lipid profiles characterized by decreased activity of paraoxonase-1, an enzyme essential for HDL metabolism. We hypothesized that SZ is accompanied by dysfunctional HDL existence and physiological disturbances in some areas of brain, passively involved in SZ pathogenesis (
Figure 9).
Spectrum of lipids in ACC reflects tiny focuses of necrosis or local myelin damage, leading to immunological misbalance and decreasing anti-oxidative activity consequently. It might be also considered as a risk factor of cardiovascular diseases in patients with SZ. We hope that this current study will help reveal a linkage between lipid balance and pathogenesis of psychiatric disorders.
4. Materials and Methods
4.1. Participants of the Study
The study was conducted on patients with schizophrenia (F20 according to version 10 of the International Statistical Classification of Diseases) in the course of psychotic decompensation admitted to the In-Patient Unit for Adults and In-Patient Unit for Adolescents at the Psychiatry Department of the University Hospital in Krakow. The study group was comprised of 22 men, 18 women; age range 15–38; mean age 22.68 ± 7.39. Patients were recruited from January 2019 to January 2020. The study was conducted in accordance with the moral, ethical, regulatory, and scientific principles governing clinical research. The study was conducted according to the guidelines of the Declaration of Helsinki and approved by the Bioethics Committee of the Jagiellonian University protocol 1072.6120.152.2019 of 27 June 2019, 1072.6120.17.2020 of 27 February 2020 and 1072.6120.252.2021 of 17 January 2022. Patient data and results of diagnostic tests were stored and processed in an anonymous form. Each patient participating in the study gave informed consent to participate in the planned research and received a protocol with a detailed description and plan of the study. At any stage of the study, the participant was allowed to withdraw from the research study. None of the respondents took advantage of this possibility. The control group has been presented by 30 volunteers aged between 18 and 40 (17 women and 13 men; average age 29.5 ± 5.33 years) without any psychiatric diseases. The characteristics of these groups were described previously by Śmierciak et al. [
37].
4.2. The Assessment of the Clinical Status and Pharmacotherapy
Each participant of the study obtained demographic data, a detailed medical history, perinatal and early childhood history, data about hereditary diseases, the presence of accompanying somatic diseases, and previously used pharmacotherapy or illegal drugs. Symptoms of psychosis in the group of people with psychotic decompensation were assessed using the PANSS diagnostic scale of positive and negative symptoms [
38]. This scale is consisting of four subscales: positive symptoms scale (P); negative symptoms scale (N); general psychopathology scale (G); and scale describing the total result (T). In the differential diagnosis group, the clinical state was assessed by a physician and a psychologist based on the presented symptoms in accordance with ICD-10.
4.3. Pharmacotherapy
Of note, 32 patients received monotherapy, and 8 patients received two-drug polytherapy. The most commonly used drug in monotherapy was haloperidol (18 patients). It was also used in 5 cases of polytherapy. The second most frequently used monotherapy drug was olanzapine. Quetiapine (2 patients), aripiprazole (2 patients), and risperidone (2 patients) were also used as monotherapy. In four cases of polytherapy, olanzapine was added to haloperidol and in one case to aripiprazole. In single patients there were combinations of quetiapine with aripiprazole, olanzapine with quetiapine, and olanzapine with aripiprazole. Drug doses were converted to chlorpromazine equivalents. Chlorpromazine equivalent (CPZE) is defined as a drug dose that corresponds to 100 mg of an oral dose of chlorpromazine [
43]. A drug equivalent to 200–300 mg of chlorpromazine is considered a minimally effective dose, while more than 1000 mg of chlorpromazine is considered high. None of the patients experienced side effects.
4.4. Metabolic Profiles
Peripheral blood samples were collected by clot-activating gel-containing serum separator tubes at the laboratory of the University Hospital in Krakow Poland and processed before 8 a.m. on the same day. All participants fasted for 8–12 h before a blood test. Routine analyses were performed using XN-2000 automated analyzers (Sysmex Corp., Kobe, Japan) as well as Cobas 6000 and Cobas 8000 biochemical analyzers (Roche HoldinG, Basel, Switzerland)/(Roche Diagnostics, Mannheim, Germany). Routine blood laboratory tests included blood morphology, lipid profile: triglycerides (TG), total cholesterol, high-density lipoproteins (HDL), low-density lipoproteins (LDL), C-reactive protein (CRP), ionogram (K+, Na+, Mg2+), and glucose.
4.5. Measurement of the Activity of Paraoxonase 1 (PON-1) in the Blood
The enzymatic activity of paroxonase was assessed by method of Eckerson et al. with own modification described in our previous paper [
35,
43].
4.6. Neuroimaging Analysis
The study used magnetic resonance imaging (MRI) with a 1.5 T magnetic field induction MR system and an 8-channel head coil in a horizontal position to obtain images of the brain. A standard MR brain examination protocol was used, which included sequences for FLAIR, T1-weighted, T2-weighted, and diffusion-weighted imaging (DWI). Assessment of brain morphology was performed in order to exclude pathological or congenital lesions. Additional analysis of diffusion in the ACC region was performed using the Functool (version 7.0) image analysis software (the version 7.0) (GE Healthcare; Chicago, IL, USA) [
31]. During this study, the standard protocol for MRI of the head in force at the University Hospital in Krakow was used. This is already written in version 495–496. The PRESS sequence was used to select the region of interest in spectroscopy (described in version 502–507). The MR system was equipped with firm whole-body gradients that provided an amplitude of 33 mT/m and a rising rate of 120 T/m/s on each axis, which allowed for highly repeatable, fast, and accurate scans. Two-dimensional T2-weighted images were acquired in sagittal, axial, and coronal planes to show the position of the volume of interest (VOI) and anatomical brain structures for spectroscopy.
Magnetic resonance spectroscopy (MRS) was performed using the single-voxel technique (SVS) with a point-resolved spectroscopy sequence (PRESS) and chemical shift selective imaging sequence (CHESS) for water suppression. Automatic shimming was used to achieve satisfying spectra, which is an automatic procedure to improve the homogeneity of the magnetic field after a patient is placed in it and applies to the volume of the selected voxel (voxel shimming). During the project, MRS signal was obtained from three locations situated symmetrically in the anterior cingulate cortex (ACC), right and left frontal lobes, centered on the interhemispheric fissure and parallel and superior to the dorsal anterior surface of the corpus callosum. The VOI reached approximately 8 cm3 and was adapted to the anatomical size of the location where the spectrum was obtained from. The period of the sequence lasted 2 min 12 s, and MRS acquisition specifications of 35 ms TE with 64 averages were obtained.
In the study described, MRS was used to investigate the metabolic changes in the anterior cingulate cortex (ACC) and frontal lobes of the brain. The data obtained from MRS were processed using SAGE 7.0 (Spectroscopy Analysis by GE). The processing involved reconstruction of the data, offset correction, zero filling, apodization, determination of peaks, Fourier transformation, and calculation of relative ratios of metabolite concentrations in relation to Cr.
The processing steps involved converting the Free Induction Decay (FID) signal into numerical data files containing basic (raw) data. The raw data were then reconstructed by applying filters and automatic Fourier transformation. The reconstructed data were subjected to offset correction, zero filling, and apodization to improve the signal-to-noise ratio and resolution of the spectrum. Peaks in the spectrum were identified and marked for further analysis.
The spectrum with marked peaks was then converted back into the FID signal, which was Fourier transformed to obtain the final spectrum. The area under the selected peaks was then read, and the developed spectrum was superimposed on the original spectrum to confirm the accuracy of the analysis. Finally, the relative ratios of metabolite concentrations in relation to Cr were calculated.
Metabolites were manually chosen from the spectrum: lipids (lip 0.9–1.0 ppm), lactates (lac 1.33 ppm), alanine (ala 1.8), N-acetyl-aspartate (NAA 2.02 ppm), glutamate (glu 2.1 ppm), γ-aminobutyric acid (GABA 2.3 ppm), glutamine (gln 2.45 ppm), creatine (Cr 3.02 ppm), choline (Cho 3.22 ppm), glucose (glc 3.43 and 3.8 ppm), myoinositol (mI 3.56 and 4.0 ppm), glu + gln + GSH complex (3.7 ppm), and phosphocreatine (3.9 ppm).
Diffusion imaging (DWI) was performed using EPI sequences. The EPI sequence uses two strong magnetic field gradients, called diffusion gradients. Diffusion gradients are symmetrically switched on before and after the pulse 180° in a single spin-echo sequence. The task of diffusion gradients is to distinguish between diffusing and stationary spins. The first diffusion gradient causes the spins to phase apart, the second to re-phase. If the spins cannot diffuse freely, they are affected by both diffusion gradients. As a result, the MR signal is strengthened. In the case of free diffusion, the phasing is not complete, which causes attenuation of the MR signal amplitude. The DWI sequence consisted of two acquisitions for two different values of the b factor. One acquisition was made for b = 0, the other for b = 1500 (b is a technical parameter of diffusion gradients). DWI sequence parameters are presented in
Table 9. The process of diffusion in tissues should be extended to include phenomena occurring in biostructures, such as perfusion, microcirculation, movement on a macroscopic scale (respiratory movements, heartbeat, patient movement), and movement at the tissue level (mainly related to capillary blood flow as well as tissue pulsation in the vicinity of larger arteries). All these phenomena, together with diffusion anisotropy in the brain tissue, affect the amplitude of the MR signal. Therefore, instead of the diffusion coefficient used in physics and chemistry, the term ADC is used. In addition, the parameter affecting the contrast of the DWI image is the echo time. Typically, TE = 60–120 ms is used to visualize the diffusion process in the tissue. This means that the signal in the DWI images also depends on the transverse relaxation time of the tissue. In order to obtain images that depend only on the diffusion process, the value of the apparent diffusion coefficient (ADC) was calculated for each voxel of the imaged layer. The values of the ADC coefficient for individual voxels are presented using the so-called ADC maps. The ADC map consists of pixels whose color depends on the value of the ADC coefficient. The higher the ADC value, the brighter the pixel on the ADC map, and vice versa. The value of the ADC coefficient can be determined numerically. For this purpose, additional software installed on the diagnostic station is used. The degree of orientation of the movement of water molecules, i.e., the so-called fractionated anisotropy, was examined using diffusion tensor imaging (DTI). Sequence parameters are presented in
Table 9. In order to express the degree of anisotropy of the examined structure, the fractional anisotropy (FA) coefficient was calculated. It is a scalar quantity reaching values in the range of 0–1. A value of 0 corresponds to an isotropic structure, and a value of 1 to a structure in which diffusion is only possible in one direction. Due to the degree of organization, the white matter of the brain is characterized by a high value of FA (the highest in the corpus callosum and pyramidal tracts). Gray matter is characterized by relatively low FA values. Very low (close to 0) FA values are typical for cerebrospinal fluid. MR imaging enables the measurement of the diffusion process of water molecules in human tissues, particularly the brain. The diffusion of water molecules in the white matter and spinal cord is anisotropic, while it is isotropic in the gray matter. The source of anisotropy is due to the cell membranes and the degree of myelination of fibers. With an increase in the degree of myelination (maturation) of nerve cells, there is an increase in diffusion anisotropy and a decrease in the average diffusion coefficient. These changes can be explained by an increase in myelination, a reduction in the amount of water in the brain, an increase in the cohesion and compactness of nerve fibers, and a reduction in intercellular space observed with age. In addition, damage or degeneration of nerve fibers leads to a decrease in the degree of anisotropy. Diffusing molecules move between tissue microstructures, reflecting or passing through various barriers in the form of cell membranes or cell organelles. These barriers impede the free diffusion of water molecules. The displacement of water molecules in the tissue depends on the microstructure of the tissue. A short diffusion time reflects the local viscosity of the intracellular space, while a longer time reflects the cellular barrier effect. Therefore, the measurement of the DWI signal and the ADC value reflects the tissue microstructure, and the magnitude of the ADC depends on the type of tissue. The source DWI and DTI images were quantified using FuncTool 7.0 software for the reconstruction and analysis of DICOM images on the GE Advantage Workstation 4.5 diagnostic station. The analysis of the source DWI and DTI data was carried out in the following stages: (1) entering the source DWI and DTI images into FuncTool, (2) setting the " Processing Threshold" to the maximum value to ensure that all pixels within the brain were selected for the calculation of the final ADC maps, (3) checking the value of the parameter b read from the DICOM file, (4) automatic generation of ADC and FA maps, and (5) measuring the DWI signal, ADC, and FA coefficients in particular places. The DWI, ADC, and FA values in the FuncTool software are displayed as mean values with standard deviation. The DWI, ADC, and FA values were obtained from three locations situated symmetrically in the anterior cingulate cortex (ACC), right and left frontal lobes, centered on the interhemispheric fissure and parallel and superior to the dorsal anterior surface of the corpus callosum (
Figure 7 and
Figure 8).
4.7. Statistical Analysis
Statistical analysis was performed using the IBM SPSS Statistics 25.0 package. Kruskal–Wallis test analysis allowed for the checking of whether there are statistically significant differences between more than two groups of people. When statistically significant differences occurred, an appropriate post hoc test was used. This allowed for the checking of which groups there are statistically significant differences. The selection was made on the basis of homogeneity of variance in the compared groups. In the case of comparing two groups, it was the Mann–Whitney U test. Spearman’s correlation analysis made it possible to check whether there is a statistically significant relationship between the variables studied. Regression analysis allowed to build a statistically significant model that has the greatest impact on the quality of life of the surveyed people. The value of p < 0.05 was considered statistically significant.
4.8. Limitations
The present study has several limitations that should be acknowledged. Firstly, the small group size is a result of the exploratory nature of the study. Consequently, the findings may not be generalizable to a larger population. Furthermore, the participants in the study are at different stages of illness and have experienced varying numbers of psychotic episodes. Additionally, there is a range of clinical symptom severity within the group of subjects, while the control group comprises subjects who are comparatively older. It is worth noting that due to the limited group size, it was not possible to conduct an analysis stratified by gender, which could be an important variable to consider.
Another significant limitation is the absence of analyses regarding the impact of pharmacotherapy on the pathophysiological processes being investigated. The use of neuroleptics in the study group introduces heterogeneity, as these medications have varying effects on lipid metabolism and the cardiovascular system. Moreover, potential factors that could influence oxidation and oxidative processes, such as developmental factors (e.g., birth complications), were not taken into account. The researchers also did not consider other potential confounding factors, including diet and lifestyle. Additionally, changes in body weight, BMI, and waist circumference, as well as the assessment of cardiovascular parameters, were not included in the study, which limits a comprehensive understanding of the potential relationships between the variables under investigation.