Partition dimension of COVID antiviral drug structures

: In November 2019, there was the ﬁrst case of COVID-19 (Coronavirus) recorded, and up to 3 rd of April 2020, 1,116,643 conﬁrmed positive cases, and around 59,158 dying were recorded. Novel antiviral structures of the SARS-COV-2 virus is discussed in terms of the metric basis of their molecular graph. These structures are named arbidol, chloroquine, hydroxy-chloroquine, thalidomide, and theaﬂavin. Partition dimension or partition metric basis is a concept in which the whole vertex set of a structure is uniquely identiﬁed by developing proper subsets of the entire vertex set and named as partition resolving set. By this concept of vertex-metric resolvability of COVID-19 antiviral drug structures are uniquely identiﬁed and helps to study the structural properties of structure.


Introduction
Cholera, flu and plague were the most terrifying pandemics in the past few centuries, these diseases caused millions of inhabitants of this world to die. The first incidence of COVID-19 (Coronavirus) was reported in November 2019, and by the third week of April 2020, there had been 1,116,643 confirmed positive cases and roughly 59,158 deaths. These statistics are given by the world health Organization (WHO). Not only the human health infected by this pandemic but also the economy of the world was disrupted because it spread over the world after emerging from the seafood market of Wuhan city in China [1]. The viral structure and genetic sequence of betacoronavirus (MERS-CoV) also known as novel corona or 2019-nCoV shares with the MERS-CoV which is middle eastern respiratory syndrome coronavirus. As there are some specific drugs available for this pandemic virus currently, like Pfizer. To tackle this pathogen there is an urgent need for strong antiviral agents. Researchers experimented with some existing antiviral operatives [2][3][4][5][6] and obtained some productive outcomes to tackle the transmission and infection of COVID-19. Theaflavin, hydroxychloroquine, chloroquine, thalidomide and arbidol are some antiviral compounds.
Remdesivir (GS5734) helped to prevent the infection of the Ebola virus, having a broad spectrum activity as a nucleotide analog drug [7]. It is reported in [8,9], that chloroquine is considered an antiviral drug that is also broad-spectrum. This antiviral helps to prevent autoimmune disease and malaria. This antiviral tested for the treatment of corona-virus to lower the impact of infections of fever and later on this was found helpful. By inhibiting T cell activation, hydroxy-chloroquine supposed by cytokine storm conclusively reduces the acute evolution of COVID-19. Hydroxychloroquine and chloroquine are approved by FDA as an emergency corona-virus treatment on 30 rd march of 2020, reported by Forbes [10]. The inhibitor production of corona-virus by using theaflavin as a lead compound is researched and suggested by [4]. For hepatitis C, B, A viruses and influenza, theaflavin shows a vast span of antiviral activity [11,12]. For the medical benefit of black tea, a polyphenol chemical is found liable.
By a molecular graph in this draft, we consider a transformation from a chemical structure to a molecular graph by assuming atoms and chemical bonds between them are nodes and edges respectively, and this theory is already established, for more detail, one can view some recent literature [13][14][15][16][17].
is an undirected graph of a chemical structure (network) with V (ℵ) is called as set of principal nodes (vertex set) and E (ℵ) is the set of branches (edge set). The distance between two principal nodes ζ 1 , ζ 2 ∈ V (ℵ) , denoted as d (ζ 1 , ζ 2 ) is the minimum count of branches between ζ 1 − ζ 2 path." Definition 1.2. In [18] "Suppose R ⊂ V (ℵ) is the subset of principal nodes set and defined as R = {ζ 1 , ζ 2 , . . . , ζ s }, and let a principal node ζ ∈ V (ℵ) . The identification or locations r(ζ|R) of a principal node ζ with respect to R is actually a s−ordered distances (d(ζ, ζ 1 ), d(ζ, ζ 2 ), . . . , d(ζ, ζ s )). If each principal node from V (ℵ) have unique identification according to the ordered subset R, then this subset renamed as a resolving set of network ℵ. The minimum numbers of the elements in the subset R is actually the metric dimension of ℵ and it is denoted by the term dim (ℵ) ." is the s-elements proper set and r ζ|R p = {d(ζ, R p1 ), d(ζ, R p2 ), . . . , d(ζ, R ps )}, is the s-tuple distance identification of a principal node ζ in association with R p . If the entire set of principal nodes have unique identifications, then R p is named as the partition resolving set of the principal node of a network ℵ. The least possible count of the subsets in that set of V (ℵ) is labeled as the partition dimension (pd (ℵ)) of ℵ." In the above definitions a graph or a chemical structure is shown with symbol ℵ, notation r(ζ|R) shows the position of a vertex ζ with respect to the resolving set or locating set R, and for the partition resolving set they used the symbol R p , dim (ℵ) is used for the metric dimension of a graph ℵ, partition dimension is notated by the symbol pd (ℵ) , furthermore, the notations are summarized in the Table 1.
Very few and recent literature on the topic of metrics and their generalization are given here. In [20], polycyclic aromatic compounds are discussed on the topic of metric and its generalization. A chemical structure is discussed in [21], they mentioned two-dimensional lattice is discussed with the idea of metric and of that structure. Cellulose network is considered in [22], by the same concept of distancebased theory of graph. Generalized concepts are given by [23][24][25][26]. A computer network is discussed in [27] with the concept of distance graph theory. Generalized families and structures of the graph are detailed in [28][29][30][31][32]. The partition dimension is quite a complex structure than the metric dimension, therefore, fewer exact partitions are available and bounds are presented usually. In [33], presented bounds for the partition of generalized class of convex polytopes and also in [34]. A chemical fullerene graph is presented in [35] and bounds on another chemical structure are detailed in [36], some nanotubes and sheets are presented in the form of partition sets in [37], the two-dimensional lattice structure is available in [38]. Generalized structures and classes of families of graphs are detailed in [39][40][41][42][43][44][45].
The very first use of metric dimension in 1975 by Slater [46] and he named this concept as locating set. Later in 1976, two independent researchers from the computer science field named this concept as the resolving set found in [47]. This idea is also named the metric basis in the pure mathematical study of graphs and structures, available in [48,49]. Instead of choosing a single subset from the vertex set of a graph or structure, the researchers of [49], introduced a concept in which a vertex set is completely arranged in the different disjoint subsets in such a manner to get unique identifications of vertices, and this concept is known as partition resolving set or partition dimension.
Metric dimension has many applied ways in which combinatorial optimization, robot roving, in complex games, image processing, pharmaceutical chemistry, polymer industry, and in the electric field as well. All these applications are found in [19,46,[50][51][52]. Robot roving is also attached with the concept of applications of the partitioning of a vertex set in terms of metric [50], while Djokovic-Winkler relation [53], verification, and discovery of a network, in chemistry [54], in mastermind games [55], image processing, and pattern recognition, and in hierarchical of the data structure are linked to the partition dimensions of a structure [56]. Further applications can be found in the literature of [47,57].

Main results
In this section, we will include our main results of partition locating set of some structures, for example, arbidol, chloroquine, hydroxy-chloroquine, thalidomide and theaflavin.
Given below are the node and bond set of arbidol COVID antiviral drug structure. The order (total count of nodes) and size (total count of edges) of this arbidol structure is |V (G Arbidol )| = 29, |E (G Arbidol )| = 31, respectively. Moreover, the molecular graph of Arbidol and labeling used in our main results are shown in the Figure 1. Some of the topological properties of this structure are available in the reference [58,59]. 6 19 , 9 14 , 20 28 , 17 24 , 25 27 }. Theorem 2.1. Let G Arbidol be a graph of arbidol COVID antiviral drug structure. Then the partition locating number of G Arbidol is less than or equal to four.
Proof. The partition locating number or partition dimension of graph of arbidol COVID antiviral drug structure is less than or equal to four. To prove this statement we have chosen a partition locating set with cardinality four and stated as lsp 27 }. Now to make this statement valid we have provided the representations of each node of the arbidol COVID antiviral drug structure which are given in the Table 2. Table 2. Locations of the nodes of G Arbidol .
Given locations l ( |lsp) of each node of graph of arbidol COVID antiviral drug structure is distinct and fulfill the definitions of partition locating set. This proved that the partition locating number pln (G Arbidol ) ≤ 4 of graph of arbidol COVID antiviral drug structure.
Hence, proved that pln (G Arbidol ) ≤ 4. Given below are the node and bond set of chloroquine COVID antiviral drug structure. The order (total count of nodes) and size (total count of edges) of this chloroquine structure is V G Chloroquine = 22, E G Chloroquine = 23, respectively. Moreover, the molecular graph of Chloroquine and labeling used in our main results are shown in the Figure 2. Some of the topological properties of this structure are available in the reference [58,59].  Theorem 2.2. Let G Chloroquine be a graph of chloroquine COVID antiviral drug structure. Then the partition locating number of G Chloroquine is three.
Proof. The partition locating number or partition dimension of graph of chloroquine COVID antiviral drug structure is three. To prove this statement we have chosen a partition locating set with cardinality three and stated as lsp 14 }. Now to make this statement valid we have provided the representations of each node of the chloroquine COVID antiviral drug structure which are given in the Table 3. Table 3. Locations of the nodes of G Chloroquine .
Given locations l ( |lsp) of each node of graph of chloroquine COVID antiviral drug structure is distinct and fulfill the definitions of partition locating set. This proved that the partition locating number pln G Chloroquine ≤ 3 of graph of chloroquine COVID antiviral drug structure. To make this assertion exact we need to prove that pln G Chloroquine ≥ 3 and following by contradiction we will have pln G Chloroquine = 2. Now, this is not true because this statement is reserved for path graph.
Given below are the node and bond set of hydroxy-chloroquine COVID antiviral drug structure. The order (total count of nodes) and size (total count of edges) of this hydroxy-chloroquine structure is V G Hydroxy = 23, E G Hydroxy = 24, respectively. Moreover, the molecular graph of hydroxychloroquine and labeling used in our main results are shown in the Figure 3. Some of the topological properties of this structure are available in the reference [58,59].  Proof. The partition locating number or partition dimension of graph of hydroxy-chloroquine COVID antiviral drug structure is three. To prove this statement we have chosen a partition locating set with cardinality three and stated as lsp G Hydroxy = {lsp 1 , lsp 2 , lsp 3 }, where lsp 1 = { 3 }, lsp 2 = { 14 }, and lsp 3 = V G Hydroxy \{ 3 , 14 }. Now to make this statement valid we have provided the representations of each node of the hydroxy-chloroquine COVID antiviral drug structure which are given in the Table 4. Table 4. Locations of the nodes of G Hydroxy .
0, otherwise. Given locations l ( |lsp) of each node of graph of hydroxy-chloroquine COVID antiviral drug structure is distinct and fulfill the definitions of partition locating set. This proved that the partition locating number pln G Hydroxy ≤ 3 of graph of hydroxy-chloroquine COVID antiviral drug structure.
To make this assertion exact we need to prove that pln G Hydroxy ≥ 3 and following by contradiction we will have pln G Hydroxy = 2. Now, this is not true because this statement is reserved for path graph.
Hence, proved that pln G Hydroxy = 3. Given below are the node and bond set of thalidomide COVID antiviral drug structure. The order (total count of nodes) and size (total count of edges) of this thalidomide structure is |V (G Thalidomide )| = 19, |E (G Thalidomide )| = 21, respectively. Moreover, the molecular graph of Thalidomide and labeling used in our main results are shown in the Figure 4. Some of the topological properties of this structure are available in the reference [58,59].  Proof. The partition locating number or partition dimension of graph of Thalidomide COVID antiviral drug structure is three. To prove this statement we have chosen a partition locating set with cardinality three and stated as lsp (G Thalidomide ) = {lsp 1 , lsp 2 , lsp 3 }, where lsp 1 = { 6 }, lsp 2 = { 18 }, and lsp 3 = V (G Thalidomide ) \ { 6 , 18 }. Now to make this statement valid we have provided the representations of each node of the Thalidomide COVID antiviral drug structure which are given in the Table 5. Table 5. Locations of the nodes of G Thalidomide .
Given locations l ( |lsp) of each node of graph of Thalidomide COVID antiviral drug structure is distinct and fulfill the definitions of partition locating set. This proved that the partition locating number pln (G Thalidomide ) ≤ 3 of graph of Thalidomide COVID antiviral drug structure. To make this assertion exact we need to prove that pln (G Thalidomide ) ≥ 3 and following by contradiction we will have pln (G Thalidomide ) = 2. Now, this is not true because this statement is reserved for path graph.
Given below are the node and bond set of theaflavin COVID antiviral drug structure. The order (total count of nodes) and size (total count of edges) of this theaflavin structure is |V (G Theaflavin )| = 41, |E (G Theaflavin )| = 46, respectively. Moreover, the molecular graph of Theaflavin and labeling used in our main results are shown in the Figure 5. Some of the topological properties of this structure are available in the reference [58,59].  Figure 5. Theaflavin COVID antiviral drug structure.
Theorem 2.5. Let G Theaflavin be a graph of Theaflavin COVID antiviral drug structure. Then the partition locating number of G Theaflavin is three.
Proof. The partition locating number or partition dimension of graph of Theaflavin COVID antiviral drug structure is three. To prove this statement we have chosen a partition locating set with cardinality three and stated as lsp 41 }. Now to make this statement valid we have provided the representations of each node of the Theaflavin COVID antiviral drug structure which are given in the Table 6. Table 6. Locations of the nodes of G Theaflavin .
Given locations l ( |lsp) of each node of graph of Theaflavin COVID antiviral drug structure is distinct and fulfill the definitions of partition locating set. This proved that the partition locating number pln (G Theaflavin ) ≤ 3 of graph of Theaflavin COVID antiviral drug structure. To make this assertion exact we need to prove that pln (G Theaflavin ) ≥ 3 and following by contradiction we will have pln (G Theaflavin ) = 2. Now, this is not true because this statement is reserved for path graph.
Given below are the node and bond set of Remdesivir COVID antiviral drug structure. The order (total count of nodes) and size (total count of edges) of this Remdesivir structure is |V (G Remdesivir )| = 41, |E (G Remdesivir )| = 44, respectively. Moreover, the molecular graph of Remdesivir and labeling used in our main results are shown in the Figure 6. Some of the topological properties of this structure are available in the reference [58,59].
Given locations l ( |ls) of each node of graph of Remdesivir COVID antiviral drug structure is distinct and fulfill the definitions of partition locating set. This proved that the partition locating number pln (G Remdesivir ) ≤ 4 of graph of Remdesivir COVID antiviral drug structure.
Given below are the node and bond set of Ritonavir COVID antiviral drug structure. The order (total count of nodes) and size (total count of edges) of this Ritonavir structure is |V (G Ritonavir )| = 50, |E (G Ritonavir )| = 53, respectively. Moreover, the molecular graph of Ritonavir and labeling used in our main results are shown in the Figure 7. Some of the topological properties of this structure are available in the reference [58,59]. Now to make this statement valid we have provided the representations of each node of the Ritonavir COVID antiviral drug structure which are given in the Table 8. Table 8. Locations of the nodes of G Ritonavir . Given locations l ( |ls) of each node of graph of Ritonavir COVID antiviral drug structure is distinct and fulfill the definitions of partition locating set. This proved that the partition locating number pln (G Ritonavir ) ≤ 6 of graph of Ritonavir COVID antiviral drug structure.

Conclusions
As we can see from our main results section, the partition dimension of arbidol, remdesivir is either four or less, while chloroquine, hydroxy-chloroquine, thalidomide, and theaflavin can be three subsets of their partition resolving sets. The vertex set of ritonavir can be partitioned into either six or less than six subsets. In short, this article detailed a few COVID-19 antiviral structures in the form of molecular graph theory with the metric of vertices. Moreover, the summary of the main results is given in Table 9.